Student fury as universities plan to continue online teaching into 2022 – LBC

5 July 2021, 14:15 | Updated: 5 July 2021, 15:30

Students have told LBC they are "infuriated" at plans from some universities to continue teaching parts of their course online, even as Boris Johnson is set to announce plans for all social distancing rules to be removed.

Multiple universities including Kent, Sheffield and University College London have already made public that students should expect "blended learning" - with some lectures given online.

Hundreds of students have signed a petition at Kent University after they said group lectures would continue online next year with the aim of reverting to in-person "in early 2022".

Manchester University has gone further, announcing a permanent move to including online teaching in their courses, including for "explanatory material" that would previously have been given in lecture theatres.

But despite promises of more in-person teaching, after over a year of watching lectures from their bedrooms students have told LBC they are thoroughly opposed to the plans and have little trust in university management.

Biochemistry first-year student Caitlin Wright told LBC she has only had four hours of in-person teaching in her first year at Manchester University.

"Labs have been taught by YouTube tutorials and when people went in to do one they had no idea what to do and how to use the equipment," she recounted.

Caitlin described the decision by Manchester to move to permanently include online teaching as part of the courses as "absolutely shocking and not in the best interests of students".

"I understand why it was necessary for this year but past the pandemic I am not sure why it is necessary.

"Everyone learns so much better in person, where they can bounce ideas off each other and put their hands up to ask questions. Online it takes three to five business days to get an answer to your question."

Read more: Manchester students claim police are carrying out 'random' Covid-19 checks in halls

Similarly, first-year Politics student Chris Adair told LBC he is worried the "quality of teaching will be severely affected if the university use the pandemic as an excuse to move to online teaching".

While the university says using a hybrid approach will allow students more flexibility, Chris told LBC he did not understand this as "many lectures were already recorded" pre-pandemic.

Chris said he and other students are "very, very worried" that the university could again move back to fully-online teaching.

"Last year they promised there would be blended learning and they reneged on that in the fist few weeks. There is uncertainty and real distrust between students and management."

Read more: Manchester Uni students pull down lockdown fencing put up around halls

Nick Hillman, Director of the Higher Education Policy Institute, told LBC universities have been scarred by the chaos of last autumn and are adapting their plans accordingly.

"Students regard learning as a social endeavour and see part of the university experience as spending time in the presence of people from other countries, other parts of the UK and other backgrounds," he explained.

"But universities got it wrong last year, when they promised face-to-face learning would come back earlier than it was allowed to for most students, and they are desperate not to overpromise this year."

Unlike Manchester, the University of Sheffield have not said they will be moving to blended learning permanently, but will adapt their learning to include online teaching "should this be necessary".

Sheffield say their "expectation and current plan is to deliver as much face-to-face teaching as possible in 2021-22", but students are concerned that they have heard nothing concrete from the university so far.

"I have only had 45 minutes of actually being at university, one in-person seminar the entire year," Politics student Dan Walsh told LBC.

"I would be hoping for an approach that is blended but also returns teaching to what it is meant to be," they continued.

"My course is meant to have 10 weeks of teaching but the university is saying because it is online only five weeks is needed.

"We're getting half the teaching for 9,000. That's not fair, that's not just."

Ahead of Boris Johnson's announcement that all sectors of the economy will now be able to open up, Dan added: "What difference is it going to make if we don't have in-person teaching if everyone is going to the pubs and clubs. It's pretty futile."

Explained: What time is Boris Johnson's announcement and what will he say?

Responding to the student's concerns, a University of Manchester spokesperson told LBC: This is not online teaching, but aboutaugmenting in-person lectures, seminars, labs, Q&As and discussions, and workshops with high quality online materials for self-study.

"We have been speaking to students for some time about ways to increase flexibility and choice and we will continue to do so to help shape this activity to their needs and the needs of each discipline.

"Our commitment to blended and flexible learning is part of the university strategy.

A University of Sheffield spokesperson said they "are working hard to provide the best on-campus experience in a Covid-secure way, in line with government guidelines.

Our top priority is always the wellbeing of our university community. Our expectation and current plan is to deliver the great majority of teaching face-to-face in September, with some larger lectures being delivered online.

"However, we have proven expertise in providing blended learning over the past year and will be able to adapt our learning and teaching delivery in response to new Covid-19 safety measures should this be needed.

"Digital delivery has opened up many possibilities for enhanced innovative learning and virtual social activities over the past year.

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Student fury as universities plan to continue online teaching into 2022 - LBC

Mibelle debuts new moss based ingredient to harmonize the skin’s moisture flow – Premium beauty

A few years after the launch of MossCellTec No.1, the Swiss-based supplier of cosmetic ingredient is launching MossCellTec Aloe[1], an unequaled aloe-moss extract sustainably obtained.

Derived from aloe-moss (Aloina aloides), a tiny dark green to reddish-brown moss measuring 2 to 5 mm in height and known as common aloe-moss, MossCellTec Aloe improves cell-to-cell communication via connexin channels, optimally evens the moisture distribution in the skin and reduces the volume and depth of wrinkles.

Due to the similarity in the appearance of the leaves, aloe-moss was named after the Aloe vera plant. This rare and tiny moss species has a high water retention capacity. Compared to seed plants, mosses do not have roots and water transport systems. Instead, they absorb water directly into their leaves. Mosses can trap excess water and nutrients from the soil and air.

In vivo tests have shown that MossCellTec Aloe can reduce signs of skin aging (skin elasticity, wrinkle volume and depth), improve skin hydration and improve moisture homogeneity.

MossCellTec Aloe is based on Mibelle Biochemistrys MossCellTec technology which allows for the sustainable large-scale production of the moss extract.

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Mibelle debuts new moss based ingredient to harmonize the skin's moisture flow - Premium beauty

New Plant Growth Regulator Thins Stone Fruit and Apples – Growing Produce

Valent BioSciences LLC announces EPA registration of a new plant growth regulator (PGR), which will be marketed under the brand name Accede, utilizing the active ingredient 1-aminocyclopropane-1-carboxylic acid (ACC).

Accede is the first PGR based on a naturally occurring compound developed specifically for thinning of stone fruit, including peaches and nectarines. It also gives apple growers an effective tool to thin apples in the late thinning window when fruit are 15 mm to 20 mm in diameter. According to Valent BioSciences, until now, no fruit thinner has provided reliable thinning at this stage of development. Use of Accede will reduce the need for costly hand thinning to adjust the crop load and generate higher fruit quality and grower returns.

ACC occurs naturally in plants. Once applied to the crop, the active ingredient in Accede is quickly converted to ethylene using the plants natural biochemical pathways. The ethylene generated after application of Accede stimulates and accelerates flower and fruit drop in apples and stone fruit.

Accede does not leave ACC residues at harvest, as it is rapidly broken down in plants. The product was classified as a biochemical by the EPA in 2015. The technology in Accede is covered by numerous patents.

This game-changing plant growth regulator will revolutionize the way tree fruit growers manage their crop loads, Dr. Warren Shafer, Vice President of Global Research and Development and Regulatory Affairs at Valent BioSciences, says. Its registration in the U.S. is the culmination of more than a decade of research and development collaboration between Valent BioSciences, Valent U.S.A. LLC, and our parent company, Sumitomo Chemical Co., Ltd. We are proud to bring this unique, effective biorational product to market and help growers realize its tremendous benefits.

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New Plant Growth Regulator Thins Stone Fruit and Apples - Growing Produce

Climate change means Kansas farmers are dealing with hotter nights and change in rainfall and freezing patterns – The Topeka Capital-Journal

By Brian Grimmett| Kansas News Service

MANHATTAN Climate change conjures notions of rising water levels along the coasts, severe drought in the Intermountain West and the record temperatures baking the Pacific Northwest this week.

Add to that toasty Kansas evenings.

New research from Kansas State University shows that rising overnight temperatures hurt wheat harvests. Rice, corn and barley all face similar problems.

While researchers also look into finding more resilient varieties of those crops to account for the change, the immediate climate trends could have a dramatic impact.

In trials of some of the most popular varieties of wheat grown in Kansas, K-State and North Carolina State University researchers found that an increase of only 1.8 degrees Fahrenheitin overnight temperatures caused a 5% reduction in wheat yield.

Most people think plants arent dynamic, but they are, said Colleen Doherty, an associate professor of biochemistry at North Carolina State University. Plants are constantly regulating their biological processes gearing up for photosynthesis just before dawn, winding that down in the late afternoon, determining precisely how and where to burn their energy resources.

She said their experiments showed that hotter overnight temperatures confuse the plants internal clock. With a screwed-up clock, the plant has a harder time turning the sugars produced during photosynthesis in the day into plant growth.

The amount of wheat that youll get will go down, but also the quality of wheat will go down, said K-State crop physiologist Krishna Jagadish. So your bread probably may start to taste a little bit different in the future.

Average summer nighttime temperatures have been increasing across the state. Since 1970, the average low in the Wichita area has increased 2.7 degrees. In Topeka, it increased 3.5 degrees.

At the same time, the average summer high temperature only increased 1.4 degrees in Wichita and 2.8 degrees in Topeka.

Jagadish said its harder for people to notice these changes when the average temperature is increasing more during the night than it is in the day. But researchers, like him, are beginning to look more into the issue and to provide information that reveals the true extent of the dangers.

Rising overnight temperatures arent the only negative impacts from climate change that Kansans can expect to experience. Assistant state climatologist Mary Knapp says were already seeing changes in precipitation patterns.

Were getting more rain, but it may not be distributed as evenly as needed, she said.

That means some places are going from very dry to getting the expected monthly rain total in a single day. That wont show up in long-term averages, but has real consequences.

Youve got more of it running off, she said. Youve got more erosion issues and youve got more flooding issues.

Knapp also said Kansas winters are getting milder. She said the state will still experience its typical spring freezes in March and April, but milder Decembers and Januarys will confuse trees and plants, making them less resilient to those freezes.

Its not all doom and gloom from the wheat research. Theres already evidence that some varieties of wheat are more resilient to temperature increases in both the day and the night. Jagadish said once those traits have been genetically identified, scientists can begin breeding new varieties that combine that trait with other proven varieties.

It is going to take time, he said. But I think thats the way to do it and we are making progress.

The researchers suspect the sensitivity to rising nighttime temperatures can be found in all starchy grains. Theyve now turned their attention to corn, to prove their hypothesis.

(Our study) is not just an interesting scientific question, Doherty said. Its a global food security issue.

Brian Grimmett reports on the environment, energy and natural resources for KMUW in Wichita and the Kansas News Service.

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Climate change means Kansas farmers are dealing with hotter nights and change in rainfall and freezing patterns - The Topeka Capital-Journal

Portable Veterinary Biochemistry Analyzer Market Global Demand, Research and Top Leading Player to 2026 Covid-19 Analysis KSU | The Sentinel…

Global Portable Veterinary Biochemistry Analyzer Market report provides information on types, applications and its regional markets including past and expected Opportunities. Portable Veterinary Biochemistry Analyzer Market report delivers data on Manufacturers, Geographical Regions, Types, Applications, Key Drivers, Challenges, Opportunities, Annual Growth Rate, Market Share, Revenue and the actual process of whole Portable Veterinary Biochemistry Analyzer industry.

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BEAT THE PANDEMIC WITH THE RESEARCH FORETELL (Download Complimentary Covid-19 document on Global Portable Veterinary Biochemistry Analyzer Market)

The scope of this research report extends from the basic outline of the Portable Veterinary Biochemistry Analyzer Market to tricky structures, classifications and applications. This research report also provides a clear picture of the global market by presenting data through effective information graphics. It also provides a detailed list of factors that affect market growth.

A detailed study of the competitive landscape of the Global Portable Veterinary Biochemistry Analyzer Market has been given along with the insights of the companies, financial status, trending developments, mergers & acquisitions and SWOT analysis. This research will give a clear and precise idea about the overall market to the readers to take beneficial decisions.

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This report contains market size and forecasts of Portable Veterinary Biochemistry Analyzer in global, including the following market information:

Global Portable Veterinary Biochemistry Analyzer Market Revenue, 2016-2021, 2022-2027, ($ millions)

Global Portable Veterinary Biochemistry Analyzer Market Sales, 2016-2021, 2022-2027, (K Units)

Global top five Portable Veterinary Biochemistry Analyzer companies in 2020 (%)

The global Portable Veterinary Biochemistry Analyzer market was valued at xx million in 2020 and is projected to reach US$ xx million by 2027, at a CAGR of xx% during the forecast period.

MARKET MONITOR GLOBAL, INC (MMG) has surveyed the Portable Veterinary Biochemistry Analyzer manufacturers, suppliers, distributors and industry experts on this industry, involving the sales, revenue, demand, price change, product type, recent development and plan, industry trends, drivers, challenges, obstacles, and potential risks.

Total Market by Segment:

Global Portable Veterinary Biochemistry Analyzer Market, By Type, 2016-2021, 2022-2027 ($ Millions) & (K Units)

Global Portable Veterinary Biochemistry Analyzer Market Segment Percentages, By Type, 2020 (%)

Automatic

Semi-Automatic

Global Portable Veterinary Biochemistry Analyzer Market, By Application, 2016-2021, 2022-2027 ($ Millions) & (K Units)

Global Portable Veterinary Biochemistry Analyzer Market Segment Percentages, By Application, 2020 (%)

Veterinary Hospitals

Veterinary Clinics

Others

Global Portable Veterinary Biochemistry Analyzer Market, By Region and Country, 2016-2021, 2022-2027 ($ Millions) & (K Units)

Global Portable Veterinary Biochemistry Analyzer Market Segment Percentages, By Region and Country, 2020 (%)

North America

US

Canada

Mexico

Europe

Germany

France

U.K.

Italy

Russia

Nordic Countries

Benelux

Rest of Europe

Asia

China

Japan

South Korea

Southeast Asia

India

Rest of Asia

South America

Brazil

Argentina

Rest of South America

Middle East & Africa

Turkey

Israel

Saudi Arabia

UAE

Rest of Middle East & Africa

Competitor Analysis

The report also provides analysis of leading market participants including:

Key companies Portable Veterinary Biochemistry Analyzer revenues in global market, 2016-2021 (Estimated), ($ millions)

Key companies Portable Veterinary Biochemistry Analyzer revenues share in global market, 2020 (%)

Key companies Portable Veterinary Biochemistry Analyzer sales in global market, 2016-2021 (Estimated), (K Units)

Key companies Portable Veterinary Biochemistry Analyzer sales share in global market, 2020 (%)

Further, the report presents profiles of competitors in the market, key players include:

EKF Diagnostics

Samsung

Randox

Alphatecscientific

Genrui

KPM Analytics(AMS Alliance)

Woodleyequipment

Idexx

Zoetis(Abaxis)

Seamaty

YSENMED

MNCHIP

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Key Features of the Report:

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Portable Veterinary Biochemistry Analyzer Market Global Demand, Research and Top Leading Player to 2026 Covid-19 Analysis KSU | The Sentinel...

biochemical diagnostic reagent Market Report Examines Business Opportunity and Worldwide Scope by Forecast 2021 to 2026 The Courier – The Courier

A new report titled, Global biochemical diagnostic reagent Market has been added into its vast repository by Straits Research. The report analyzes and estimates the biochemical diagnostic reagent market on a global, regional, and country level. The report offers data of previous years along with an in-depth analysis from 2017 to 2022 on the basis of revenue (USD Billion). Besides, the report offers a comprehensive analysis about the factors driving and restraining the growth of the market coupled with the impact they have on the demand over the forecast period. In addition, the report includes the study of lucrative opportunities available in the biochemical diagnostic reagent market on a global level.

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TheMajorPlayers Covered in this Report:RocheBeijing Strong BiotechnologiesRandoxSiemens HealthineersFosunPharmaBeckman CoulterSysmexBeijing Leadman BiochemistryBioSinoDojindo LaboratoriesKAINOS LaboratoriesDAAN Gene

The report on the Global biochemical diagnostic reagent Market offers data of previous years along with in-depth analysis from 2021 to 2027 on the basis of revenue (USD Billion). Besides, the report offers a comprehensive analysis of the factors driving and restraining the growth of the market coupled with the impact they have on the demand over the forecast period.

biochemical diagnostic reagent Market By Types

Liquid Double ReagentDry Powder Double Reagent

biochemical diagnostic reagent Market By Applications

HospitalClinicLaboratory

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This report forecasts revenue growth at the global, regional, and local levels and provides an analysis of the most recent industry trends from 2021 to 2027 in each of the segments and sub-segments. In addition, the report highlights the impact of COVID-19 on the Global biochemical diagnostic reagent Market and how the market is undertaking measures to reduce the losses. Some of the major geographies included in the market are given below:

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RocheBeijing Strong BiotechnologiesRandoxSiemens HealthineersFosunPharmaBeckman CoulterSysmexBeijing Leadman BiochemistryBioSinoDojindo LaboratoriesKAINOS LaboratoriesDAAN Gene

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biochemical diagnostic reagent Market Report Examines Business Opportunity and Worldwide Scope by Forecast 2021 to 2026 The Courier - The Courier

Turning Yeast Cells Into Labs For Studying Drivers of Gene Regulation – NC State News

Researchers have developed a more efficient platform for studying proteins that play a key role in regulating gene expression. The approach uses engineered yeast cells to produce enzyme and histone proteins, conduct biochemical assays internally, and then display the results.

Biomedical and biotech researchers are interested in the mechanisms that allow histones to regulate gene activity, says Alison Waldman, first author of a paper on the work and a Ph.D. student at North Carolina State University. But the conventional tools for histone research are unwieldy and slow. We wanted to develop something faster and less expensive and we did.

In complex organisms, chromosomes are largely made up of DNA and a group of proteins called histones. These histones are important for packing the DNA into chromosomes properly, but also play a role in regulating gene expression. In other words, they help determine when and how specific genes are turned on or off.

One of the features that makes histones challenging to study is that they often have chemical modifications that, alone or in combination, alter the role the histone plays in gene expression.

Histones essentially serve as docking sites for other proteins that influence gene expression, and the chemical modifications we see on histones play a role in determining which proteins have access to a given gene, says Balaji Rao, co-corresponding author of the paper and a professor of chemical and biomolecular engineering at NCState.

And to make matters more complicated, this is a dynamic process. A histone may have no modifications, it may retain a modification for the entire life of the cell, or modifications may be added and removed repeatedly. There is, in short, a lot going on. And enzymes are the catalysts responsible for all of those changes. Basically, enzymes are the mechanism for attaching or removing histone modifications.

So if you really want to understand whats going on with histones, you have to understand the chemical modifications. But if you want to understand the chemical modifications, you need to understand which enzymes are present and what they are doing.

Conventional methods for understanding how enzymes modify a histone involve using one of two techniques. First, you could use chemical synthesis to create enzymes and histone proteins, then conduct an assay in a test tube to see what happens. Second, you could genetically engineer one bacteria to produce an enzyme and engineer other bacteria to produce histone proteins, then harvest the relevant proteins, purify them, then conduct an assay to see what happens.

Our technique uses a genetically modified yeast cell to produce both the enzyme and the histone, Waldman says. The chemical modification takes place within the cell, and the resulting modified histone is sent to and displayed on the surface of the cell.

In other words, the yeast cell makes the relevant proteins, does the assay for you, and then displays the result on top, says Albert Keung, co-corresponding author of the work and an assistant professor of chemical and biomolecular engineering at NCState.

The modified yeast platform is significantly faster than conventional techniques. For example, examining a single enzyme/histone pairing would take a couple days, instead of a week.

But its easier to scale up than existing techniques, so you would save substantially more time if you were looking at a lot of proteins, Keung says.

In addition, there are some proteins that cant be made using chemical synthesis, or that cant be purified, Rao says. Our technique doesnt require chemical synthesis or purification, which means we can look at proteins that were difficult or impossible to assay in the past.

The researchers demonstrated the utility of the technique by having engineered yeast cells produce two types of histones and a well-studied enzyme called p300, which adds a specific acetyl group modification to histones.

Weve shown that our technique works, Waldman says. The next step is to begin expanding the modifications were looking at and scaling up the process.

The paper, Mapping the Residue Specificities of Epigenome Enzymes by Yeast Surface Display, is published in the journal Cell Chemical Biology. The work was done with support from the National Science Foundation, under grant 1830910; and the National Institutes of Health, under grant R21EB023377.

-shipman-

Note to Editors: The study abstract follows.

Mapping the Residue Specificities of Epigenome Enzymes by Yeast Surface Display

Authors: Alison C. Waldman, Balaji M. Rao and Albert J. Keung, North Carolina State University

Published: June 28, Cell Chemical Biology

DOI: 10.1016/j.chembiol.2021.05.022

Abstract: Histone proteins are decorated with a combinatorially and numerically diverse set of biochemical modifications. Here we describe a versatile and scalable platform which enables efficient characterization of histone modifications without the need for recombinant protein production. As proof-of-concept, we first used this platform to rapidly profile the histone H3 and H4 residue writing specificities of the human histone acetyltransferase, p300. Subsequently, a large panel of commercially available antiacetylation antibodies for their specificities, identifying many suitable and unsuitable reagents. Further, enabled efficient mapping of the large binary crosstalk space between acetylated residues on histones H3 and H4 and uncovered previously unreported residue interdependencies affecting p300 activity. These results show that using yeast surface display to study histone modifications is a useful tool that can advance our understanding of chromatin biology by enabling efficient interrogation of the complexity of epigenome modifications.

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Turning Yeast Cells Into Labs For Studying Drivers of Gene Regulation - NC State News

Massive Growth of Biochemical Reagents Market by 2027 | Roche Holding AG, Thermo Fisher Scientific Inc., Siemens Healthineers, Abbott Laboratories …

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Biochemical Reagents Market research report is the new statistical data source added by A2Z Market Research.

Biochemical Reagents Market is growing at a High CAGR during the forecast period 2021-2027. The increasing interest of the individuals in this industry is that the major reason for the expansion of this market.

Biochemical Reagents Market research is an intelligence report with meticulous efforts undertaken to study the right and valuable information. The data which has been looked upon is done considering both, the existing top players and the upcoming competitors. Business strategies of the key players and the new entering market industries are studied in detail. Well explained SWOT analysis, revenue share and contact information are shared in this report analysis.

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Top Key Players Profiled in this report are:

Roche Holding AG, Thermo Fisher Scientific Inc., Siemens Healthineers, Abbott Laboratories, Agilent Technologies, Inc., Bio-Rad Laboratories, Merck and Co. Inc., Johnson and Johnson, Waters Corporation, BD.

The key questions answered in this report:

Various factors are responsible for the markets growth trajectory, which are studied at length in the report. In addition, the report lists down the restraints that are posing threat to the global Biochemical Reagents market. It also gauges the bargaining power of suppliers and buyers, threat from new entrants and product substitute, and the degree of competition prevailing in the market. The influence of the latest government guidelines is also analyzed in detail in the report. It studies the Biochemical Reagents markets trajectory between forecast periods.

Global Biochemical Reagents Market Segmentation:

Market Segmentation by Type: Cell and Tissue Culture Reagents, Chromatography Reagents, Electrophoresis Reagents, Polymerase Chain Reaction (PCR) Reagent Kits, Other.

Market Segmentation by Application: Hospitals, Diagnostic Centers, Academics and Research, Pharma and Biotech Companies.

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Regions Covered in the Global Biochemical Reagents Market Report 2021: The Middle East and Africa (GCC Countries and Egypt) North America (the United States, Mexico, and Canada) South America (Brazil etc.) Europe (Turkey, Germany, Russia UK, Italy, France, etc.) Asia-Pacific (Vietnam, China, Malaysia, Japan, Philippines, Korea, Thailand, India, Indonesia, and Australia)

The cost analysis of the Global Biochemical Reagents Market has been performed while keeping in view manufacturing expenses, labor cost, and raw materials and their market concentration rate, suppliers, and price trend. Other factors such as Supply chain, downstream buyers, and sourcing strategy have been assessed to provide a complete and in-depth view of the market. Buyers of the report will also be exposed to a study on market positioning with factors such as target client, brand strategy, and price strategy taken into consideration.

The report provides insights on the following pointers:

Market Penetration: Comprehensive information on the product portfolios of the top players in the Biochemical Reagents market.

Product Development/Innovation: Detailed insights on the upcoming technologies, R&D activities, and product launches in the market.

Competitive Assessment: In-depth assessment of the market strategies, geographic and business segments of the leading players in the market.

Market Development: Comprehensive information about emerging markets. This report analyzes the market for various segments across geographies.

Market Diversification: Exhaustive information about new products, untapped geographies, recent developments, and investments in the Biochemical Reagents market.

Table of Contents

Global Biochemical Reagents Market Research Report 2021

Chapter 1 Biochemical Reagents Market Overview

Chapter 2 Global Economic Impact on Industry

Chapter 3 Global Market Competition by Manufacturers

Chapter 4 Global Production, Revenue (Value) by Region

Chapter 5 Global Supply (Production), Consumption, Export, Import by Regions

Chapter 6 Global Production, Revenue (Value), Price Trend by Type

Chapter 7 Global Market Analysis by Application

Chapter 8 Manufacturing Cost Analysis

Chapter 9 Industrial Chain, Sourcing Strategy and Downstream Buyers

Chapter 10 Marketing Strategy Analysis, Distributors/Traders

Chapter 11 Market Effect Factors Analysis

Chapter 12 Global Biochemical Reagents Market Forecast

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Massive Growth of Biochemical Reagents Market by 2027 | Roche Holding AG, Thermo Fisher Scientific Inc., Siemens Healthineers, Abbott Laboratories ...

Considerations for Tracer Selection to Assess Biochemical Recurrence in Prostate Cancer – Cancer Network

Raoul S. Concepcion, MD, FACS: Dr Ghesani, educate us. You deal with this a lot, and you understand. You have a tracer, and then there are nuances to this based on half-life. Gallium has a particular half-life, and F-18 [fluorine-18] has a particular half-life. Obviously, choline has a particular half-life. How does that impact and how does that play out potentially, as these scans are made more available to the general practitioner, the community urologist and oncologist? What are the factors there that the practitioners need to know that are the nuanced differences between thosetracers?

Munir Ghesani, MD: I would like to make 2 more points that I just started thinking about as Brian and Judd mentioned those items. I would like to add on those as well. As Brian referenced, there are data that show theres less than 20% sensitivity for combination of bone scans and CT [computerized tomography] scans in the setting of biochemical recurrence. Theres even a bigger problem, which is that in the small minority of the patients where the scans pick up the disease, its misleading because it does not fully clarify the extent of disease. Therefore, if you superficially look at it, you will see about 20% or less benefit. But in fact, even a subgroup of those patients does not benefit because their disease has not been properly delineated. They may have disease that was picked up only in part by the CT and bone scans, and you may end up targeting your treatment and not recognizing that there may be disease outside what the CT and bone scan did not pick up.

For that reason, it will be important to work with the CMS [Centers for Medicare & Medicaid Services] and other providers, and we are aggressively working in various societies by collaborating with one another to make these points clear. Hopefully, soon, these requirements for bone scans and CT scans will not be there. The second point I wanted to mention was in that polling question, the item about other, and this brings back to your question about all different options. There is also fluorine-18 FDG [fluorodeoxyglucose], which is the most used agent for most other cancers. It has been shown that for most cancers in the prostate it does not work, but with a very high Gleason score, they have very high level of glucose metabolism. Therefore, in a select and small subgroup of patients who have known to have a very high Gleason score, when they recur, one should also consider the possibility of FDG PET [positron emission tomography scan] or CT because in that subgroup, it is going to be very powerful.

Regarding your question about how we should choose. At the current level, the fluorine-18 half-life of 2 hours is readily available all around. It will be easy for the sides. Even after bone scan and CT scans have been negative, you have gone through the peer-to-peer and have an approval of fluciclovine, which would be the most used agent across the country at this time. For those sites that have the availability of gallium PSMA [prostate-specific membrane antigen] through the cross-referencing IND [investigational new drug] or clinical trials, but those would be mostly major academic centers. They can consider using gallium or fluorine PSMA-based agents. For small sitesthe Mayo Clinic, for examplewhere the C-11 choline was first developed, they can with cyclotron availability produce in a large batch, and we know that sites like the Mayo Clinic are doing a large number of carbon-11 PSMA scans.

Raoul S. Concepcion, MD, FACS: That is a limitation, isnt it? The half-life of the C-11 is so short that they cant

Munir Ghesani, MD: Its 20 minutes.

Raoul S. Concepcion, MD, FACS: You cant ship it a distance. To any of you, we know that fluciclovine Axumin is approved. It is approved in patients who have been treated for prostate cancer and have a rising PSA [prostate-specific antigen]. Correct me if Im wrong, but doesnt that include patients on active surveillance whose PSA [is rising]? Can you make the argument that active surveillance is a treatment and if they have a rising PSA, you could get fluciclovine? Have any of you tried that?

Brian Helfand, MD, PhD: You can make that argument. I dont think its correct. Ive seen it done, and its not really the FDA indication. What they mean is that interventions with curative intent, or subsequent hormone therapy that the patient is progressing. However, active surveillance was not part of that initial approval indication. Having said that, in the world many things are done whether theres evidence or not evidence for that. Therefore, we dont generally monitor our active surveillance patients with that.

Raoul S. Concepcion, MD, FACS:Perfect.

Transcript edited for clarity.

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Considerations for Tracer Selection to Assess Biochemical Recurrence in Prostate Cancer - Cancer Network

IIT Madras researchers find new method to make AIDS drug more effective – Business Today

Researchers at the Indian Institute of Technology, Madras claim to have found a novel way to make HIV/AIDS drugs more effective. The findings of their study, published in Biochemistry, the peer-review Journal of the American Chemical Society, say that introducing electrostatic interaction sites on potential drug molecules can enhance the efficacy of the antiviral drug against the HIV virus. The research was led by Prof. Sanjib Senapati, Department of Biotechnology, IIT Madras, along with research scholars Mohammed Ahsan and Chinmai Pindi.

"Current inhibitors (molecules that bind with the enzyme, thereby making it unavailable to the virus for growth and maturation) that target HIV-1 protease (HIVPR, an essential enzyme that is used by the AIDS virus for growth and maturation), make use of the weak forces of attraction called 'van der Waal's forces' to attach themselves to the protease molecule. Given that these forces are weak, the efficacy of the drug is variable and the virus will soon become resistant to them," Prof. Senapati, says.

The Molecular Dynamics (MD) simulation studies conducted by IIT Madras researchers showed the presence of a strong and asymmetrical electric charge in the active site of the HIVPR. If a drug molecule can be designed with a complementary charge, so that it can bind tightly with this active site through electrostatic attraction, it can permanently deactivate/inhibit the enzyme, they felt.

"Current drugs lack this electrostatic complementarity. This must be investigated because it is well-known that electrostatic forces between molecules are much stronger than van der Waals forces," Prof. Senapati said.

The researchers propose that drug design strategies should embrace both electrostatics and van der Waals interactions to complement the HIVPR active site architecture. Further, the team believes that such compounds will be effective against both wild-type and resistant HIV variants. According to them, it is a paradigm-shifting idea and will offer a whole new approach to the development of drugs for HIV-AIDS.

Prof. Chandra Verma, who has a Ph.D. from Bioinformatics Institute, A*STAR, Singapore, and is not involved in this IIT Madras Research, predicts a bright future for HIV drug development, with such knowledge base.

AIDS is one of the most devastating diseases and is a major cause of death among youth in many parts of the world. Since its outbreak nearly four decades ago, tremendous efforts have been directed towards development of antiretroviral therapies that target different stages in the life cycle of the virus that causes this deadly disease.

Also read: India issues fresh Covid-19 guidelines for travellers from UK, Brazil, South Africa

Also read: BT Business Leaders of TN: Manufacturing, electronics, SaaS can make India $5 trillion economy, say experts

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IIT Madras researchers find new method to make AIDS drug more effective - Business Today

Global Biochemical Methane Market 2020 Size Share Upcoming Trends Segmentation And Forecast To 2026 – The Courier

The report aims to provide a high-quality and concise overview of the globalBiochemical Methane market, taking into account demand trends, competitive intelligence and technological challenges and developments, and other important topics. The cleverly crafted market analysis helps market players to understand the most important developments affecting their business in the global Biochemical Methane industry. Readers can become conscious of the vital opportunities on the global market for Biochemical Methane including the important aspects that drive and arrest business growth. The research study also offers an in-depth geographical overview of the global market of Biochemical Methane and focuses on important concepts and solutions that market players should concentrate on for robust growth.

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Research Coverage:This is the first part of the research that covers market segmentation outlines, years studied, analysis targets, major global Biochemical Methane manufacturers, and product range.Overview:The report here puts the spotlight on market output, revenue, usage, and potential. It also brings market trends, drivers, restraints and macroscopic indicators to light.Profiles of companies:This section includes a broad examination of key players in the global Drug for Ulcerative Colitis market based on various factors such as the latest advances, market share and gross margins. This provides an analysis of SWOT, too.Regional Production:All the regions evaluated in the study are examined here based on key factors such as volume, sales, market share, import, and export.Regional demand:Each domestic market discussed here is evaluated based on the global markets share of sales and output.Product market penetration: comprises the study of costs, sales and industry overview by product type.

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Immunic, Inc. Announces Positive Top-Line Data From Investigator-Sponsored Phase 2 Proof-of-Concept Clinical Trial of IMU-838 in Primary Sclerosing…

NEW YORK, Feb. 18, 2021 /PRNewswire/ --Immunic, Inc. (Nasdaq: IMUX),a clinical-stage biopharmaceutical company developing a pipeline of selective oral immunology therapies aimed at treating chronic inflammatory and autoimmune diseases, today announced positive top-line data from an investigator-sponsored phase 2 proof-of-concept clinical trial of IMU-838 in primary sclerosing cholangitis (PSC). This single-arm, open-label, exploratory study was designed to investigate IMU-838's potential to improve various biochemical parameters in PSC patients and help determine whether any such activity warrants further investigation in randomized PSC trials. As previously announced, due to the COVID-19 pandemic, only 18 of the targeted 30 patients were enrolled in the study (intent-to-treat population, ITT), of whom only 11 patients completed the full IMU-838 treatment course and were evaluable over the 24-week treatment period (per-protocol population, PP).

The PP population experienced a statistically significant decrease in serum alkaline phosphatase (ALP) levels (p=0.041) after 24 weeks of treatment using 30 mg IMU-838 once daily, as compared to baseline. A consistent individual pattern of a stable decrease in ALP values was observed in the PP population between baseline and week 24, without any single patient showing an increase of more than 20% of ALP. As per the definition of the primary objective of the study, 27.3% of the patients in the PP population had a clinically relevant reduction of serum ALP higher than 25% at week 24, without an increase in liver biochemistry of more than 33%, as compared to baseline. Biochemical endpoints, such as changes in serum ALP, have been used in PSC trials performed by third parties.

Regarding the secondary objectives of the study, no changes in aspartate aminotransferase (AST), alanine aminotransferase (ALT), or total, direct or indirect bilirubin were observed in the ITT or PP populations, as compared to baseline. In addition, despite the limited scope of the data, encouraging results were observed regarding symptoms of inflammatory bowel disease, a common comorbidity for PSC patients, and patient assessments of health-related quality of life. The study also found that IMU-838 is a safe and well-tolerated oral drug for PSC patients and treatment-emergent adverse events were rare and generally mild.

"I am very excited about the effects we have seen in this highly underserved patient population where there is only a small number of cases worldwide and where no pharmaceutical treatment option is currently available," noted Daniel Vitt, Ph.D., Chief Executive Officer and President of Immunic. "We are also very pleased to see that IMU-838's safety and tolerability profile was confirmed in this patient group. The results from this small, open-label study suggest that IMU-838 merits further clinical testing in PSC. We are in discussions with investigators and leading clinical experts to further evaluate the data set and to explore potential next steps for this indication."

"Currently, no effective treatment options are available for PSC patients and the hepatology community is very keen to see new approaches and clinical programs for the investigation of promising new approaches. I am grateful that Mayo Clinic and Immunic are collaboratively exploring this underserved indication for which liver transplantation is often the only effective option," stated Keith Lindor, M.D., Professor of Medicine Emeritus and former President of the American Association for the Study of Liver Diseases. "Although we are mindful of the small size of this dataset, I do believe the results are noteworthy and merit further exploration. Notable in this small patient cohort is the absolute consistency with which these patients experienced decreases in serum alkaline phosphatase at the 24-week time point."

Study Background and Baseline Characteristics

The single-arm, open label, exploratory study was an investigator-sponsored trial led by Elizabeth Carey, M.D., Professor of Medicine, Division of Gastroenterology and Hepatology, Department of Internal Medicine, Mayo Clinic, who had received Investigator Investigational New Drug (IND) approval from the U.S. Food & Drug Administration (FDA) and had been granted Institutional Review Board (IRB) approval to conduct the study. The study was supported by a grant from the National Institutes of Health (NIH) and was conducted at two sites: Mayo Clinic, Phoenix, Arizona (Dr. Carey) and Mayo Clinic, Rochester, Minnesota (John E. Eaton, M.D.), both of which are tertiary referral centers for PSC patients.

The study, for which Immunic provided the study medication, planned to enroll 30 patients with PSC, aged 18 to 75 years, who received 30 mg of IMU-838 once daily for a period of 24 weeks. Enrollment for the study took place between July 2019 and September 2020, but almost all enrollment occurred in 2019 and early 2020. During the COVID-19 pandemic, recruitment for this study was hampered, as patients with PSC are at a high risk of COVID-19 infections and were advised to avoid travel and unnecessary social contacts such as those required to participate in a clinical trial. Together with the investigators, Immunic determined to readout data of the 18 patients who were enrolled prior to the COVID-19 pandemic. The ongoing COVID-19 pandemic also triggered the principal investigator's decision to terminate the study in late 2020, before the intended recruitment goal of 30 patients was reached.

A total of 18 patients started treatment of 30 mg IMU-838 once daily (intent-to-treat population, ITT, n=18). Of these 18 patients, 11 patients received the full 24-week treatment with IMU-838 (per-protocol population, PP, n=11). Due to the high number of discontinued patients during the COVID-19 pandemic and the fact that all discontinued patients in an ITT statistical analysis will be counted as treatment failures at week 24, this analysis focuses mainly on the 11-patient PP population.

Primary Objective

The primary objective of this study was to determine whether IMU-838 reduces serum ALP in adult patients diagnosed with PSC. The main analysis for the primary objective was whether patients could achieve a reduction of ALP at week 24 which is greater or equal to 25%, as compared to baseline, while the AST increase at week 24 is no more than 33%, as compared to baseline. This positive primary outcome was achieved by 3 of 11 patients in the PP population (27.3%, 95% CI: 6-61%). By virtue of inclusion criteria, patients at baseline had to have an elevated ALP value of at least 1.5 times upper limit of normal (ULN).

In addition, time from baseline was calculated as a continuous variable and treated as the primary predictor using a random intercept model which was adjusted for age at baseline and gender. For this longitudinal analysis of ALP from baseline to week 24 in the PP population, the ALP value statistically significantly (p=0.041) decreased by an average of 5.76 IU/L every 30 days (95% CI: -11.29, -0.23; statistical model). The time trend was not statistically significant in the ITT analysis (p=0.578) due to missing data following the high rate of treatment discontinuations during the COVID-19 pandemic.

Secondary Objectives

Secondary objectives were to investigate the liver biochemistry parameters, AST, ALT, and total/direct/indirect bilirubin, as well as the concentrations of proinflammatory cytokines, as compared to baseline. The longitudinal analysis of both AST and ALT as well as total, direct and indirect bilirubin values showed a stable pattern in the PP population with no statistically significant change over time and the confidence interval to include the no-change scenario (AST: average 30 day change 1.22 IU/L, 95% CI: -0.53, 2.97, p=0.170; ALT: average 30 day change 0.85 IU/L, 95% CI -1.46, 3.15, p=0.467, total bilirubin: average 30 day change 0.00 mg/dL, 95% CI -0.01, 0.02, p=0.561, direct bilirubin: average 30 day change 0.00 mg/dL, 95% CI -0.01, 0.01, p=0.861, indirect bilirubin: average 30 day change 0.00 mg/dL, 95% CI -0.01, 0.01, p=0.556). Similar results were found in the ITT population. In addition, a decrease in the Ulcerative Colitis Clinical score was observed in evaluated patients, although the number of assessed patients was limited.

"This was a feasibility study to explore activity of IMU-838 in PSC patients based on biochemical parameters. IMU-838 was found to lead to a statistically significant reduction of serum ALP over time in the PP population, while no trend for increases in ALT, AST or bilirubin was observed," commented Andreas Muehler, M.D., Chief Medical Officer of Immunic. "Despite the challenges we faced due to COVID-19, which severely hindered the enrollment at the two Mayo Clinic sites and which led to an unusually high discontinuation rate and an early termination of the study, we have seen encouraging activity signals for IMU-838 in this patient population. Based on these promising data and, in particular, the improvement in biochemical liver parameters, we will continue to evaluate the potential of IMU-838 as a treatment option for PSC patients. It may also be worthwhile to optimize dose levels of IMU-838 in PSC patients in the future."

For more information on this clinical trial, please visit: http://www.clinicaltrials.gov, NCT03722576.

Conference Call and Webcast Information

As previously announced, Immunic's management team will host a public conference call and webcast today, February 18, 2021 at8:00 a.m. Eastern Timeto discuss the data from the main phase 2 analysis of the CALVID-1 trial of IMU-838 in hospitalized patients with moderate COVID-19, as well as data from the investigator-sponsored phase 2 clinical trial of IMU-838 in primary sclerosing cholangitis.

To participate in the conference call, dial 1-877-870-4263 (USA) or 1-412-317-0790 (International) and ask to be joined into the Immunic, Inc. call. A live, listen-only webcast of the conference call can be accessed at https://www.webcaster4.com/Webcast/Page/2301/39950or on the "Events and Presentations" section of Immunic's website at ir.imux.com/events-and-presentations.

An archived replay of conference call and webcast will be available approximately one hour after the completion for one year on Immunic's website at: ir.imux.com.

About Primary Sclerosing Cholangitis (PSC) PSC is a rare liver disease with a prevalence of approximately 4.15 per 100,000 in the United States, in which the bile ducts in the liver become inflamed, narrow and prevent bile from flowing properly. The exact cause and disease mechanism of PSC are still unknown, but an autoimmune mechanism may play a role. There is an association with inflammatory bowel diseases, most often with ulcerative colitis and less commonly with Crohn's disease. PSC is a progressive disease and, other than liver transplantation, there are currently no approved therapies that have been shown to improve survival in patients with PSC. The estimated time from diagnosis of PSC to death or liver transplant has been shown to be less than 15 years.

About IMU-838IMU-838 is an orally available, next-generation selective immune modulator that inhibits the intracellular metabolism of activated immune cells by blocking the enzyme dihydroorotate dehydrogenase (DHODH). IMU-838 acts on activated T and B cells while leaving other immune cells largely unaffected and allows the immune system to stay functioning, e.g. in fighting infections. In previous trials, IMU-838 did not show an increased rate of infections compared to placebo. In addition, DHODH inhibitors, such as IMU-838, are known to possess a host-based antiviral effect, which is independent with respect to specific virus proteins and their structure. Therefore, DHODH inhibition may be broadly applicable against multiple viruses. IMU-838 was successfully tested in two phase 1 clinical trials in 2017 and is currently being tested in a phase 2 trial in patients with ulcerative colitis. In the third quarter of 2020, the company reported positive results from its phase 2 EMPhASIS trial of IMU-838 in relapsing-remitting multiple sclerosis, achieving both primary and key secondary endpoints with high statistical significance. In the first quarter of 2021, Immunic announced that IMU-838 has shown evidence of clinical activity in its phase 2 CALVID-1 trial in hospitalized patients with moderate COVID-19. Also, in the first quarter of 2021, the company reported positive top-line data from an investigator-sponsored phase 2 proof-of-concept clinical trial of IMU-838 in primary sclerosing cholangitis which was conducted in collaboration with Mayo Clinic. To date, IMU-838 has been tested in more than 800 individuals and has shown an attractive pharmacokinetic, safety and tolerability profile. IMU-838 is not yet licensed or approved in any country.

About Immunic, Inc.Immunic, Inc. (Nasdaq: IMUX) is a clinical-stage biopharmaceutical company witha pipeline of selective oral immunology therapies aimed at treating chronic inflammatory and autoimmune diseases, including relapsing-remitting multiple sclerosis, ulcerative colitis, Crohn's disease, and psoriasis. Immunic is developing three small molecule products: its lead development program,IMU-838, is a selective immune modulator that inhibits the intracellular metabolism of activated immune cells by blocking the enzyme DHODH and exhibits a host-based antiviral effect; IMU-935 is an inverse agonist of RORt; and IMU-856 targets the restoration of the intestinal barrier function. For further information, please visit: http://www.imux.com.

Cautionary Statement Regarding Forward-Looking StatementsThis press release contains "forward-looking statements" that involve substantial risks and uncertainties for purposes of the safe harbor provided by the Private Securities Litigation Reform Act of 1995. All statements, other than statements of historical facts, included in this press release regarding strategy, future operations, future financial position, future revenue, projected expenses, prospects, plans and objectives of management are forward-looking statements. Examples of such statements include, but are not limited to, statements relating to Immunic's three development programs and the targeted diseases; the potential for IMU-838 to safely and effectively target diseases; the proof-of-concept study of IMU-838 for the treatment of patients with primary sclerosing cholangitis; the timing of current and future clinical trials; the potential for IMU-838 as a treatment for primary sclerosing cholangitis that may be supported by the investigator-sponsored phase 2 proof-of-concept trial data, and any clinical trials, collaborations and approvals relating to such potential treatment; the nature, strategyand focus of the company; and the development and commercial potential of any product candidates of the company. Immunic may not actually achieve the plans, carry out the intentions or meet the expectations or projections disclosed in the forward-looking statements and you should not place undue reliance on these forward-looking statements. Such statements are based on management's current expectations and involve risks and uncertainties. Actual results and performance could differ materially from those projected in the forward-looking statements as a result of many factors, including, without limitation, the COVID-19 pandemic, risks and uncertainties associated with the ability to project future cash utilization and reserves needed for contingent future liabilities and business operations, the availability of sufficient resources to meet business objectives and operational requirements, the fact that the results of earlier studies and trials may not be predictive of future clinical trial results, the protection and market exclusivity provided by Immunic's intellectual property, risks related to the drug development and the regulatory approval process and the impact of competitive products and technological changes. A further list and descriptions of these risks, uncertainties and other factors can be found in the section captioned "Risk Factors," in the company's Annual Report on Form 10-K for the fiscal year ended December 31, 2019, filed with the SEC on March 16, 2020, the company's Quarterly Report on Form 10-Q for the quarter ended September 30, 2020, filed with the SEC on November 6, 2020, and in the company's subsequent filings with the Securities and Exchange Commission. Copies of these filings are available online at http://www.sec.gov or ir.imux.com/sec-filings. Any forward-looking statement made in this release speaks only as of the date of this release. Immunic disclaims any intent or obligation to update these forward-looking statements to reflect events or circumstances that exist after the date on which they were made. Immunic expressly disclaims all liability in respect to actions taken or not taken based on any or all the contents of this press release.

Contact Information

Immunic, Inc. Jessica BreuHead of Investor Relations and Communications+49 89 2080 477 09[emailprotected]

US IR ContactRx Communications GroupPaula Schwartz+1 917 322 2216[emailprotected]

US Media ContactKOGS CommunicationEdna Kaplan+1 781 639 1910[emailprotected]

SOURCE Immunic, Inc.

http://www.immunic-therapeutics.com

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Electrolyte and Biochemistry Analyzers Market is slated to grow rapidly in the forthcoming years with Top Leading Players y, z etc., etc The Bisouv…

This report also covers the impact of COVID-19 on the global market. The pandemic caused by Coronavirus (COVID-19) has affected every aspect of life globally, including the business sector. This has brought along several changes in market conditions.

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Market segment by TypeElectrolyte AnalyzersBiochemistry Analyzers

Market segment by ApplicationHospitalClinicLabsOthers

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Electrolyte and Biochemistry Analyzers Market is slated to grow rapidly in the forthcoming years with Top Leading Players y, z etc., etc The Bisouv...

Trending Report on Biochemical Diagnostic Reagent Market Business Insights and Development Analysis from 2020-2027 | Top Players Siemens…

Recent Industry trends & research observe on Global Biochemical Diagnostic Reagent Market 2020 & Forecast 2027 highlights various agency elements like types, end-users, programs. The competitive landscape view in Biochemical Diagnostic Reagent Industry, mergers & acquisitions, research, new technologies & upcoming Biochemical Diagnostic Reagent companies are pro-Report Sheet. The market size, modern employer trends, government policies, & investment opportunities in the Biochemical Diagnostic Reagent Industry are covered.

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Dr. Joseph Angel de Soto named the Editor & Chief of the Journal of Advanced Biochemistry and Research – Martinsburg Journal

GERRARDSTOWN Dr. Joseph Angel de Soto, of Gerrardstown, has been named editor and chief of "The Journal of Advanced Biochemistry and Research."

He is currently the editor of "Virology Research & Reports." Dr. Soto received his doctorate in medicine and a Ph.D. in pharmacology from Howard University. His dissertation was titled, The Treatment of Breast Cancer with Chemo-hormonal Therapy. He also completed doctoral studies in national security and intelligence.

His clinical medical training was at Howard University Hospital and Washington Hospital Center. He then completed his fellowship at the National Institutes of Health in pharmacogenomics and translational oncology, where he was the fellow of the year.

He has published over 150 articles and papers. As a professor, he has been faculty of the year seven times. De Soto also received the ASCO Cancer Researcher of the Year award. According to the publishers of "The Journal of Advanced Biochemistry and Research," he is considered one of the top physician-scientist and pharmacogeneticists in the world.

For more information, visit the Journal of Advanced Biochemistry and Research website: https://snipub.com/journal-of-advanced-biochemistry/editorial-board-journal-of-advanced-biochemistry/.

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Dr. Joseph Angel de Soto named the Editor & Chief of the Journal of Advanced Biochemistry and Research - Martinsburg Journal

Biochemistry professor Tansey discovers protein that could melt tumors – The Vanderbilt Hustler

The discovery of MYC-HCF1 interactions may lead to a future tumor-shrinking treatment.

Vanderbilt University Medical Center (VUMC), pictured above, manages more than 2 million patients each year and is one of the largest academic medical centers in the Southeast, according to its website. (Hustler Multimedia/Truman McDaniel)

On Jan. 8, a study published in the journal eLIFE by Vanderbilt professor of biochemistry and cell and developmental biology, Dr. William Tansey, detailed the discovery of a genetic mutation that can be applied to shrink tumors quite quickly.

The protein, called MYC, is used by animals and humans alike for cell division and cell growth, which also allows tumor cells to rapidly expand. Tumors typically form when cells no longer have control of their growth, and MYC often enables cells to grow out of control, creating tumors. When Tansey and colleagues discovered a particular mutation that blocks the interaction between MYC and another protein, Host Cell Factor-1 (HCF1), tumors rapidly shrunk.

The next step, according to Tansey, is to identify certain molecules that are able to bind to HCF1 to prevent it from interacting with MYC.

Now that we know what we have to go after, the question is if we can do this beneficially and safely, Tansey said.

If molecules that bind to HCF1 are able to be identified, clinical trials could begin within the next decade for a potential tumor-melting clinical drug in the distant future, according to Tansey. However, the process is often long, and it may take years before this discovery is manifested into a drug, per Tansey.

If you had a molecule that was able to bind to HCF1 and prevent it from being touched by MYC, then that could form the basis of a future anti-cancer drug, Tansey said.

This discovery is the second time that a cancer-treating drug was discovered at Vanderbilt. In 2015, Vanderbilt professor of biochemistry, pharmacology and chemistry, Stephen Fesik, alongside Tansey, discovered a protein named WDR5 that similarly halts interactions with MYC. WDR5 is expected to be in clinical trials shortly, and is currently supported by the National Cancer Institutes Experimental Therapeutics Program, according to Tansey.

We are looking for something that will treat pre-existing tumors, and it seems as if this discovery could lead down that path, Tansey said.

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Biochemistry professor Tansey discovers protein that could melt tumors - The Vanderbilt Hustler

Biochemical Clues Reveal How Some Corals Resist Bleaching From Climate Change That Is Killing Coral Reefs – SciTechDaily

A comparison of resistant (left) and bleached (right) corals. Credit: Courtesy of Ty Roach (HIMB)

Climate change is bleaching and killing corals, but researchers from Michigan State and the University of Hawaii are investigating how some can stand up to a warming world.

Coral reefs are beautiful and diverse ecosystems that power the economies of many coastal communities. Theyre also facing threats that are driving their decline, including the planets warming waters.

This threat hit extreme levels in 2015, when high temperatures were turning corals white around the globe. Kaneohe Bay in Hawaii was hit hard; nearly half of its corals bleached.

Hidden in the aftermath of this extreme event, however, were biochemical clues as to why some corals bleached while others were resistant, information that could help reefs better weather warming waters in the future. These clues have now been uncovered by researchers at Michigan State University and the University of Hawaii at Manoa.

It was kind of horrifying, said coral biologist Crawford Drury, who witnessed 2015s bleaching event from Florida before joining UH Manoas Hawaii Institute for Marine Biology, or HIMB. Its disheartening to watch, but I try to think of it as an opportunity.

How this disturbing event became an opportunity is now clear thanks to a February 8, 2021, report in Nature Ecology & Evolution that showcases HIMBs stewardship and MSUs biochemical expertise.

Coral samples were analyzed by mass spectrometry to investigate biochemical differences. Credit: Courtesy of Ty Roach (HIMB)

The researchers discovered chemical signatures in the corals biology, or biomarkers, that are present in organisms that were most resistant to the bleaching. This previously hidden insight could help researchers and conservationists better restore and protect reefs around the world.

Usually, we think of biomarkers as signatures of disease, but this could be a signature of health, said MSUs Robert Quinn, an assistant professor in the Department of Biochemistry and Molecular Biology. This could help us restore reefs with the most resistant stock.

Corals are symbiotic communities where coral animal cells build homes for algae that provide them energy and create their colors. When corals bleach, however, the algae are lost and leave behind skeletons that are susceptible to disease and death.

This symbiosis also plays a role in a corals resistance and resilience to bleaching, which HIMB was in a unique position to investigate literally. The institute sits right next to the reef, enabling experiments in real time.

The reef is about 100 feet away, Drury said. I could be there in 30 seconds.

During the 2015 bleaching event, researchers in the Gates Coral Lab at HIMB had tagged individual corals to keep tabs on them. Because most of the corals recovered, the team could follow them over time.

We think about it as a biological library, said Drury, the principal investigator with the Gates Coral Lab. It was set up by researchers in our lab who knew it would be very valuable.

A view of coral reefs near Hawaiis shores, where bleaching was prevalent in 2015. Credit: Photo courtesy of Ty Roach (HIMB)

Following the bleaching, the team compared and contrasted coral samples in the wild, noting how the organisms responded and recovered, making some surprising observations along the way. For example, neighboring corals could behave completely differently in response to high temperatures. One coral could bleach completely while its neighbor maintained a healthy golden hue.

To understand why, Drury and HIMB postdoctoral researcher Ty Roach, the lead author of the study, sent samples to Quinn at MSU. Here, Quinn and his team could thoroughly analyze the biochemicals of corals collected from this biological library using a method called metabolomics.

Im known more for my medical work, said Quinn, who studies the biochemistry of health and disease in humans. But Ive always loved ocean science. My background is in marine microbiology.

If the coral samples are the books in the library, Quinns lab used sophisticated equipment to reveal the biochemical language within. In particular, his team used tools known as mass spectrometers to understand what set resistant corals apart from susceptible ones.

The corals are completely different in their chemistry, but you cant tell until you run the mass spec, Quinn said. These mass specs are some of the most advanced technology on the planet.

Quinns team found that corals that were resistant to bleaching and those that were susceptible hosted two different communities of algae. The distinguishing feature between these algal populations was found in their cells, in compounds known as lipids.

The researchers metabolomic analysis detected two different lipid formulations. Bleaching-resistant corals featured algae that have what are known as saturated lipids. Susceptible corals had more unsaturated lipids.

This is not unlike the difference between oil and margarine, the latter having more saturated fat, making it solid at room temperature, Quinn said.

This discovery poses all sorts of new questions for researchers: How do the corals get these different algae? Is this difference unique to Hawaiian corals or can it be found elsewhere? How can researchers promote the growth and proliferation of resilient corals in a warming world?

Mass specs are such incredible machines and reveal intricate details of the chemistry involved. The biology is really the hard part. Quinn said. Were working on new grants. There are so many avenues to explore.

This initial project was funded by the Paul G. Allen Family Foundation.

This collaboration has been a great opportunity to ask and answer questions, Drury said. Hopefully, were just getting started.

In the meantime, having this chemical information is promising for coral conservation. When conservationists reseed corals to help restore reefs, they can potentially select more resilient specimens.

We can use natural resilience to better understand, support, and manage coral reefs under climate change, Drury said.

Conservation biology has some of the more successful stories in modern scientific history, Quinn said, pointing to the resurgence of elk in Virginia and bald eagles in Michigan. Someday, maybe we can add corals to that list.

Reference: Metabolomic signatures of coral bleaching history by Ty N. F. Roach, Jenna Dilworth, Christian Martin H., A. Daniel Jones, Robert A. Quinn and Crawford Drury, 8 February 2021, Nature Ecology and Evolution.DOI: 10.1038/s41559-020-01388-7

Funding: Paul G. Allen Family Foundation

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Biochemical Clues Reveal How Some Corals Resist Bleaching From Climate Change That Is Killing Coral Reefs - SciTechDaily

Alumnae Key to Nationwide Work on COVID-19 Vaccine – Kettering University News

Four alumnae specializing in documentation, chemical testing, quality control and software analysis have joined the fight against COVID-19.

The women Aubrie (Hoffman) Eaton, Mia (Jonascu) Hillaker, Debra (Pratt) Piper and Katie (Esch) VandeBerg all work at Par Pharmaceutical in Rochester, Mich., and apply their skills learned while they were students at Kettering University to the production of various sterile injectable products, including a potential vaccine for COVID-19.

Par Sterile began production on NVX-CoV2373, a protein-based COVID-19 vaccine candidate from Novavax, Inc. in September 2020. In December, Novavax announced the initiation of Phase 3 clinical trials in the United States and Mexico, and in January announced highly encouraging efficacy results from trials taking place in the United Kingdom and South Africa.

Its very humbling, said Quality Control Chemist VandeBerg (17, Chemistry). Its nice to know that were part of the effort attempting to make a difference in the fight against COVID and how its being treated.

Its not the front line, but its close to it in light of the fact that we are involved with the production of a potential COVID-19 vaccine, she added. Its very cool to be working on something that may have a big impact in our history.

Science, Safety and Steps to Save Lives

VandeBerg, who has been with the company since October 2017, conducts tests on raw materials before they head to production.

We put a lot of good time and effort into making sure its done the right way every time, VandeBerg said.

Materials then head to Senior Scientist Eaton (14, Biochemistry), who is responsible for chemical testing at various stages of production and completion to ensure the product meets safety standards and performs as it should.

It has been interesting. Its been moving very quickly, Eaton said. The assumption is fast means reckless, and that upsets me. There is a high level of integrity in the scientific field with defined processes and procedures. The FDA doesnt just approve things.

Eaton has been at Par Pharmaceutical since September 2020. She said this work has given her a sense of purpose.

We are by no means on the front lines, but its important to recognize that we, scientists, are very focused on working on solutions to protect those heroes, Eaton said.

Neither Eatons nor VandeBergs jobs could be done without the work of Scientist Debra Piper (13, Biochemistry). She supports the laboratory by implementing the software and analysis systems used with the testing equipment to ensure they are used appropriately and efficiently.

Piper started working at Par as part of Kettering Co-op as a student. There until 2016, she worked elsewhere for four years but returned to Par in the spring of 2020.

Its a great feeling to know your job may actually have an impact on people, and what youre doing is going toward a common cause we all want to support, Piper said. It makes you respect your job more and enjoy your job more.

Documenting Success

However, these jobs cant be done without documentation, and thats where Hillaker (18, Applied Biology) comes in.

Hillaker, who is a Quality Document Associate for a little more than a year, ensures that documents needed for the process are correct so that all standards are met. Some of the documents include labels, testing forms and batch forms, which in the simplest terms, are similar to recipe cards for products.

It feels a little bit surreal, just because I go to work every day and think, Oh my goodness, my signature is going to be on some of these very crucial documents, she said.

Like her co-workers, Hillaker recognized the potential impact her job has on society.

The whole experience overall has been crazy, but wonderful, she said. The hours have been crazy, the workload has been crazy, but at the same time, it could help the greater good in a way that I wasnt expecting.

Piper has been able to do much of her work remotely, while Hillaker, Eaton and VandeBerg have been on site. Schedules were shifted to reduce the number of people in the facility at any one time to meet COVID-19 guidelines.

Kettering Mindset and Co-op Experience Give Valuable Advantage

The women said their time at Kettering University not only connects them, but has armed them with the skills and mindset to be successful in their jobs.

Ketterings slogan was Think Differently, Eaton said. I have found that I ask different sorts of questions because my mind thinks of several possibilities instead of the direct route. I have noticed when I ask questions, people say, Ive never thought about that. Its coming at things from different angles.

VandeBerg, Hillaker and Piper cited their Kettering Co-op experiences as great preparation for life after graduation. Piper said being able to enter the industry at a younger age than your counterparts from other colleges is a valuable advantage.

You can go to school and work at the same time and apply what youre learning while youre working, she said. It really teaches you how to excel in the workforce.

Hillaker said she knew it would be a good fit for her current job because of how much she enjoyed the elements of her Co-op experience as a scribe for the Hurley Medical Center.

I was kind of surprised in the ways that Kettering prepared me, she said. I was more prepared for the medical field, but through my Co-ops and research, I found that I liked the more technical side of it and computer science part. I really enjoyed working with the data and data models and attention to detail that you get with scribing.

Eaton and Piper said they appreciated the smaller classes, too.

A lot of these upper-level classes are very, very difficult, and once you get [to upper level] chemistry, class sizes were six to nine people, Eaton said. You dont have that in other college experiences.

She said the small classes allowed her to work with the entire class to study and prepare, and made her feel as if the professor was part of her team.

Piper echoed Eatons sentiments, noting there were four or five people from her discipline in her graduating class.

I think one of the things I enjoyed the most was when the four or five of us got together to hang out, work on school work and teach each other the lessons, Piper said. We all wanted to succeed together. There wasnt competition for who was going to be the best; we all wanted to be successful together and that was something I was able to do at Kettering. I think at larger schools youre not able to get that.

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Alumnae Key to Nationwide Work on COVID-19 Vaccine - Kettering University News

Non-Lethal Biochemical Weapons Market hits USD2.32 Bn by 2028 with Taser International Manufacturing Company, Combined Systems, The Safariland Group,…

The Non-Lethal Biochemical Weapons Market is expected to exhibit a CAGR of +8% to reach US$2.32 bn by the end of 2028.

Non-Lethal Chemical Weapons. The US military is currently engaged in several research efforts to develop non-lethal chemical and biological weapons. These weapons can be placed into two main categories: incapacitants and anti-material agents.

Bacillus anthracis bacteria, which causes anthrax, is one of the most deadly agents to be used as a biological weapon. It is classified by the US Centres for Disease Control and Prevention (CDC) as a Category A agent, posing a significant risk to national security.

The use of biological weapons is prohibited under customary international humanitarian law, as well as a variety of international treaties. The use of biological agents in armed conflict is a war crime.

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North Carolina State University: Biochemical Sensor Researcher Makes MIT Technology Review’s List Of Top Young Innovators – Patch.com

Amay J. Bandodkar, an assistant professor of electrical and computer engineering at North Carolina State University, has been named one of MIT Technology Review's "Innovators Under 35" for his work on developing wearable biochemical sensors.

"I am very excited that Tech Review is recognizing our work to move health technology into the future," says Bandodkar. "I owe it to my amazing team members and mentors."

The annual list, which Tech Review has issued since 1999, was created to highlight exceptionally talented young innovators from around the world in a variety of fields. Previous winners include Mark Zuckerberg, Larry Page, Sergey Brin and Vivian Chu.

Bandodkar works at the interface of electronics, materials science, and biology to create next-generation wearable sensors with biomedical applications such as disease monitoring.

"My ultimate goal would be to develop technology that allows us to assess a person's health status by merely scanning a reader just like the tricorder from Star Trek," Bandodkar says.

Bandodkar joined NC State in January 2021, and is part of the university's National Science Foundation-funded ASSIST Center. The ASSIST Center's mission is to create self-powered, wearable health monitoring technologies.

Learn more about this year's honorees on the MIT Technology Review website here and in the July/August issue, which went live online June 30.

Founded in 1899, MIT Technology Review is an independent media company whose insight, analysis, and interviews explain the newest technologies and their commercial, social, and political impacts. MIT Technology Review's mission is to bring about better-informed and more conscious decisions about technology through authoritative, influential, and trustworthy journalism.

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This press release was produced by North Carolina State University. The views expressed here are the author's own.

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North Carolina State University: Biochemical Sensor Researcher Makes MIT Technology Review's List Of Top Young Innovators - Patch.com