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Category Archives: Transhuman News

Dr. Reddy’s sells off psoriasis candidate in out-licensing deal – BioPharma Dive

Posted: August 25, 2017 at 3:37 am

Dive Brief:

Dr Reddy's has completed Phase 3 studies, manufactured registration batches, and made preparations for a New Drug Application (NDA) filing for DFD-06, but has chosen to license the drug out rather than pursue commercialization in house.

"We look forward to obtaining NDA approval this fall, enabling Encores management team to quickly deliver this product to the providers and their patients." says Anil Namboodiripad, SVP, Proprietary Products, and president, Promius Pharma.

Dr. Reddy's has had a challenging year. Shares in the drugmaker began a month-long slide following the announcement of its first quarter 2018 results in July 2017, which recorded a 6% decline in revenues and a 53% fall in profits year-on-year. The lackluster results were due, in part, to price erosion from U.S. customer consolidation and a lower contribution from U.S. product launches.

The Indian drugmaker has also had a tough time with manufacturing, running afoul of stepped-up oversight from the Food and Drug Administration. In April, the regulator completed an audit of the company's Srikakulam-based production site, flagging points where the site fell shortof regulatory standards. This inspection resulted in a Form 483, adding to similar letters issued to the company's Miryalguda and Bachupally sites this year.

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Stanford Center Hopes to Take Stem Cell and Gene Therapies to a New Level – Sickle Cell Anemia News

Posted: at 3:37 am

The new Stanford Center for Definitive and Curative Medicine will fosterthe development ofstem cell and gene therapies for genetic diseases, including sickle cell anemia.

More than280 million people around the world have diseases with genetic causes, experts estimate. While research has identified the underlying causes of several, scientists have developed few therapies that can address the causes or cure the diseases.

Treatments have been developed thatsignificantly improve patients health, however. They include public health initiatives, targeted therapies and surgery.

Scientists believe stem cell and gene therapy can cure some genetic diseases. They would likely do this either by rewiring cells to fight a disease more efficiently or by correcting a genetic errorin a patients DNA.

Stanford not only does excellent research in disease mechanisms, cell and stem cell biology, but also promotes collaboration between its medical schools and hospitals.

The initiative is a joint venture of theStanford University School of Medicine,Stanford Health CareandStanford Childrens Health.

Dean Predicts Center Will Be Major Force in the Precision-health Revolution

The Center for Definitive and Curative Medicine is going to be a major force in theprecision-health revolution, Dr. Lloyd Minor, dean of the School of Medicine, said in a press release. Our hope is that stem cell and gene-based therapeutics will enable Stanford Medicine to not just manage illness but cure it decisively and keep people healthy over a lifetime.

We are entering a new era in medicine, one in which we will put healthy genes into stem cells and transplant them into patients,said Christopher Dawes, the president and CEO of Stanford Childrens Health. And with the Stanford Center for Definitive and Curative Medicine, we will be able to bring these therapies to patients more quickly than ever before.

The work of the center is not being done anywhere else in the country only at Stanford, said David Entwistle, president and CEO of Stanford Health Care. We have a pipeline of clinical translational therapies that the center is now driving forward, enabling us to translate basic science discoveries into state-of-the-art therapies for diseases which up until now have been considered incurable.

Dr. Maria Grazia Roncarolo will direct the center,which will be in the Department of Pediatrics.The renowned medical doctor and scientist is the George D. Smith Professor of Stem Cell and Regenerative Medicine.

It is a privilege to lead the center and to leverage my previous experience to build Stanfords preeminence in stem cell and gene therapies, said Roncarolo, who is also chief of pediatric stem cell transplantation and regenerative medicine, co-director of theBass Center for Childhood Cancer and Blood Diseases,and co-director of theStanford Institute for Stem Cell Biology and Regenerative Medicine.

Main Mission Will Be to Turn Scientific Discoveries Into Treatments

Stanford Medicines unique environment brings together scientific discovery, translational medicine and clinical treatment, Roncarolo added. We will accelerate Stanfords fundamental discoveries toward novel stem cell and gene therapies to transform the field and to bring cures to hundreds of diseases affecting millions of children worldwide.

The centers main mission will be to turn scientific discoveries into treatments. A world-classinterdisciplinary team of scientists should help it deliver on that promise.

Leaders of the team will include Dr. Matthew Porteus, an associate professor of pediatrics, and Dr. Anthony Oro, the Eugene and Gloria Bauer Professor of dermatology. Dr. Sandeep Soni will direct the centers stem cell clinical trial office.

The center will provide novel therapies that can prevent irreversible damage in children, and allow them to live normal, healthy lives, said Dr. Mary Leonard, chair of pediatrics at Stanford Childrens Health. The stem cell and gene therapy efforts within the center are aligned with the strategic vision of the Department of Pediatrics and Stanfordsprecision-healthvision, where we go beyond simply providing treatment for children to instead cure them definitively for their entire lives.

A unique feature of the center will be a close association with the Stanford Laboratory for Cell and Gene Medicine, which is working on new cell and gene therapies.

The lab has already developed genetically corrected bone marrow cells as a treatment for sickle cell anemia. Other genetically modified cells it has created include skin grafts for children with the genetic disease epidermolysis bullosa and lymphocytes for children with leukemia.

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Research reveals how estrogen regulates gene expression – Baylor College of Medicine News (press release)

Posted: at 3:37 am

Binding of steroid estrogen hormones to estrogen receptor (ER) in the cell nucleus triggers the sequential recruitment different coactivators to regulate gene transcription.

Estrogen hormones regulate gene expression. They achieve this by first binding to estrogen receptor in the cell nucleus, which triggers the recruitment of different molecules called coactivators in specific order. In a study published in Molecular Cell, a team of researchers at Baylor College of Medicine, the University of Texas MD Anderson Cancer Center and the University of Texas Health Science Center at Houston shows that the sequential recruitment of coactivators is not simply adding molecules to the complex, it results in dynamic specific structural and functional changes that are necessary for effective regulation of gene expression.

Estrogens are a group of hormones that are essential for normal female sexual development and for the healthy functioning of the reproductive system. They also are involved in certain conditions, such as breast cancer. Estrogen also plays a role in male sexual function. Estrogens carry out their functions by turning genes on and off via a multi-step process. After estrogen binds to its receptor, different coactivators bind to the complex in a sequential manner.

Experimental evidence suggests that different estrogen-receptor coactivators communicate and cooperate with each other to regulate gene expression, said corresponding author Dr. Bert OMalley, chair and professor of molecular and cellular biology and Thomas C. Thompson Chair in Cell Biology at Baylor College of Medicine. However, how this communication takes place and how it guides the sequence of events that regulate gene expression was not clear.

In this study, OMalley, Dr. Wah Chiu, Distinguished Service Professor and Alvin Romansky Professor of Biochemistry and Molecular Biology at Baylor during the development of this project, and their colleagues combined cryo-electron microscopy structure analysis and biochemical techniques and showed how the recruitment of a specific coactivator CARM1 into the complex guides the subsequent steps leading to gene activation.

For the estrogen receptor complex to be able to regulate gene expression, the coactivator CARM1 needs to be added after other coactivators have been incorporated into the complex, said first author Dr. Ping Yi, assistant professor of molecular and cellular biology at Baylor. We discovered that when CARM1 is added, it changes the complex both chemically and structurally, and these changes guide subsequent steps that lead to gene activation.

We now have a better understanding of how this molecular machine works and of what role each one of the components plays. We are better prepared to understand what might have gone wrong when the machine fails, OMalley said.

Other contributors to this work include Zhao Wang, Qin Feng, Chao-Kai Chou, Grigore D. Pintilie, Hong Shen, Charles E. Foulds, Guizhen Fan, Irina Serysheva, Steven J. Ludtke, Michael F. Schmid, Mien-Chie Hung and Wah Chiu.

Support for this study was provided by the Komen Foundation (5PG12221410), the Department of Defense (R038318-I and W81XWH-15-1-0536); National institutes of Health grants (HD8818, NIDDK59820, P41GM103832 and R01GM079429); CNIHR, R21AI122418 and R01GMGM072804; CPRIT grants (RP150648 and DP150052); and a National Cancer Institute Cancer Center Support grant (P30CA125123) to the BCM Monoclonal Antibody/recombinant Protein Expression Core Facility.

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In pain? For some, gene studies could provide a quick cure – WRAL.com

Posted: at 3:37 am

Raleigh, N.C. Many people spend years searching for a diagnosis of a debilitating medical problem, paying for treatments or surgery that don't help. Now, researchers at UNC say that, for some, recent advances in genetic testing could fix their problems once and for all.

Elizabeth Davis, a local genes study participant, does not take walking for granted. For 30 years, she could barely walk at all. "When I was 6, I started walking on my toes," she said. "I started going to different doctors, trying to find out what it was."

The muscles in Davis' foot had tightened up, causing her pain. She needed crutches and, sometimes, a wheelchair. For years, the cause of her condition remained a mystery.

According to Dr. James Evans, a researcher at UNC's Center for Genetic Medicine, about 30 percent of patients find an answer to their problems when they participate in a genes study. Participants' blood samples are analyzed with the latest advances in DNA sequencing.

"The patients themselves typically seek us out because they've been looking for answers for a long time," said Evans. "There might not be a known treatment, so sometimes that answer doesn't really change their life significantly."

Davis saw positive results after participating in the study, and Dr. Jonathan Berg, an Assistant Professor of Genetics at UNC, was happy with the results. "Her case is an unusual one in that it just happened to be a condition that is exquisitely treatable -- with just a pill," said Berg.

The genes study discovered that Davis had a muscle rigidity problem similar to that of many people with Parkinson's Disease. Doctors learned that it was Dopa, a drug used by millions of Americans with the disease, could help Davis walk again.

"The relief was fast and just by taking a quarter of a pill," said Davis. "I overheard my oldest son telling his friend that 'his mom is not on crutches anymore.' I'll never forget him saying that."

The study, funded by the National Institutes of Health, has even bigger plans for the future. UNC researchers say they're planning a randomized controlled trial to see if these types of genetic tests can benefit patients in the long run and prove to be a cost-effective diagnostic test.

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In pain? For some, gene studies could provide a quick cure - WRAL.com

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Test reveals possible treatments for disorders involving MeCP2 … – Baylor College of Medicine News (press release)

Posted: at 3:37 am

The first step consisted of genetically modifying a laboratory cell line in which the researchers could monitor the levels of fluorescent MeCP2 as they inhibited molecules that might be involved in its regulation. First author Dr. Laura Lombardi, a postdoctoral researcher in the Zoghbi lab at the Howard Hughes Medical Institute, developed this cell line and then used it to systematically inhibit one by one the nearly 900 kinase and phosphatase genes whose activity could be potentially inhibited with drugs.

We wanted to determine which ones of those hundreds of genes would reduce the level of MeCP2 when inhibited, Lombardi said. If we found one whose inhibition would result in a reduction of MeCP2 levels, then we would look for a drug that we could use.

The researchers identified four genes than when inhibited lowered MeCP2 level. Then, Lombardi and her colleagues moved on to the next step, testing how reduction of one or more of these genes would affect MeCP2 levels in mice. They showed that mice lacking the gene for the kinase HIPK2 or having reduced phosphatase PP2A had decreased levels of MeCP2 in the brain.

These results gave us the proof of principle that it is possible to go from screening in a cell line to find something that would work in the brain, Lombardi said.

Most interestingly, treating animal models of MECP2 duplication syndrome with drugs that inhibit phosphatase PP2A was sufficient to partially rescue some of the motor abnormalities in the mouse model of the disease.

This strategy would allow us to find more regulators of MeCP2, Zoghbi said. We cannot rely on just one. If we have several to choose from, we can select the best and safest ones to move to the clinic.

Beyond MeCP2, there are many other genes that cause a medical condition because they are either duplicated or decreased. The strategy Zoghbi and her colleagues used here also can be applied to these other conditions to try to restore the normal levels of the affected proteins and possibly reduce or eliminate the symptoms.

Other contributors to this work include Manar Zaghlula, Yehezkel Sztainberg, Steven A. Baker, Tiemo J. Klisch, Amy A. Tang and Eric J. Huang.

This project was funded by the National Institutes of Health (5R01NS057819), the Rett Syndrome Research Trust and 401K Project from MECP2 duplication syndrome families, and the Howard Hughes Medical Institute. This work also was made possible by the following Baylor College of Medicine core facilities: Cell-Based Assay Screening Service (NIH, P30 CA125123), Cytometry and Cell Sorting Core (National Institute of Allergy and Infectious Diseases, P30AI036211; National Cancer Institute P30CA125123; and National Center for Research Resources, S10RR024574), Pathway Discovery Proteomics Core, the DNA Sequencing and Gene Vector Core (Diabetes and Endocrinology Research Center, DK079638), and the mouse behavioral core of the Intellectual and Developmental Disabilities Research Center (NIH, U54 HD083092 from the National Institute of Child Health and Human Development).

The full study can be found inScience Translational Medicine.

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To Protect Genetic Privacy, Encrypt Your DNA – WIRED

Posted: at 3:37 am

In 2007, DNA pioneer James Watson became the first person to have his entire genome sequencedmaking all of his 6 billion base pairs publicly available for research. Well, almost all of them. He left one spot blank, on the long arm of chromosome 19, where a gene called APOE lives. Certain variations in APOE increase your chances of developing Alzheimers, and Watson wanted to keep that information private.

Except it wasnt. Researchers quickly pointed out you could predict Watsons APOE variant based on signatures in the surrounding DNA. They didnt actually do it, but database managers wasted no time in redacting another two million base pairs surrounding the APOE gene.

This is the dilemma at the heart of precision medicine: It requires people to give up some of their privacy in service of the greater scientific good. To completely eliminate the risk of outing an individual based on their DNA records, youd have to strip it of the same identifying details that make it scientifically useful. But now, computer scientists and mathematicians are working toward an alternative solution. Instead of stripping genomic data, theyre encrypting it.

Gill Bejerano leads a developmental biology lab at Stanford that investigates the genetic roots of human disease. In 2013, when he realized he needed more genomic data, his lab joined Stanford Hospitals Pediatrics Departmentan arduous process that required extensive vetting and training of all his staff and equipment. This is how most institutions solve the privacy perils of data sharing. They limit who can access all the genomes in their possession to a trusted few, and only share obfuscated summary statistics more widely.

So when Bejerano found himself sitting in on a faculty talk given by Dan Boneh, head of the applied cryptography group at Stanford, he was struck with an idea. He scribbled down a mathematical formula for one of the genetic computations he uses often in his work. Afterward, he approached Boneh and showed it to him. Could you compute these outputs without knowing the inputs? he asked. Sure, said Boneh.

Last week, Bejerano and Boneh published a paper in Science that did just that. Using a cryptographic genome cloaking method, the scientists were able to do things like identify responsible mutations in groups of patients with rare diseases and compare groups of patients at two medical centers to find shared mutations associated with shared symptoms, all while keeping 97 percent of each participants unique genetic information completely hidden. They accomplished this by converting variations in each genome into a linear series of values. That allowed them to conduct any analyses they needed while only revealing genes relevant to that particular investigation.

Just like programs have bugs, people have bugs, says Bejerano. Finding disease-causing genetic traits is a lot like spotting flaws in computer code. You have to compare code that works to code that doesnt. But genetic data is much more sensitive, and people (rightly) worry that it might be used against them by insurers, or even stolen by hackers. If a patient held the cryptographic key to their data, they could get a valuable medical diagnosis while not exposing the rest of their genome to outside threats. You can make rules about not discriminating on the basis of genetics, or you can provide technology where you cant discriminate against people even if you wanted to, says Bejerano. Thats a much stronger statement.

The National Institutes of Health have been working toward such a technology since reidentification researchers first began connecting the dots in anonymous genomics data. In 2010, the agency founded a national center for Integrating Data for Analysis, Anonymization and Sharing housed on the campus of UC San Diego. And since 2015, iDash has been funding annual competitions to develop privacy-preserving genomics protocols. Another promising approach iDash has supported is something called fully homomorphic encryption, which allows users to run any computation they want on totally encrypted data without losing years of computing time.

Megan Molteni

The Go-To Gene Sequencing Machine With Very Strange Results

Sarah Zhang

Cheap DNA Sequencing Is Here. Writing DNA Is Next

Rachel Ehrenberg, Science News

Scrubbing IDs Out of Medical Records for Genetic Studies

Kristen Lauter, head of cryptography research at Microsoft, focuses on this form of encryption, and her team has taken home the iDash prize two years running. Critically, the method encodes the data in such a way that scientists dont lose the flexibility to perform medically useful genetic tests. Unlike previous encryption schemes, Lauters tool preserves the underlying mathematical structure of the data. That allows computers to do the math that delivers genetic diagnoses, for example, on totally encrypted data. Scientists get a key to decode the final results, but they never see the source.

This is extra important as more and more genetic data moves off local servers and into the cloud. The NIH lets users download human genomic data from its repositories, and in 2014, the agency started letting people store and analyze that data in private or commercial cloud environments. But under NIHs policy, its the scientists using the datanot the cloud service providerresponsible with ensuring its security. Cloud providers can get hacked, or subpoenaed by law enforcement, something researchers have no control over. That is, unless theres a viable encryption for data stored in the cloud.

If we dont think about it now, in five to 10 years a lot peoples genomic information will be used in ways they did not intend, says Lauter. But encryption is a funny technology to work with, she says. One that requires building trust between researchers and consumers. You can propose any crazy encryption you want and say its secure. Why should anyone believe you?

Thats where federal review comes in. In July, Lauters group, along with researchers from IBM and academic institutions around the world launched a process to standardize homomorphic encryption protocols. The National Institute for Standards and Technology will now begin reviewing draft standards and collecting public comments. If all goes well, genomics researchers and privacy advocates might finally have something they can agree on.

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‘South Park’ Is Getting An Epic Eight-Day Marathon In September – Konbini US

Posted: at 3:36 am

America's favorite comedy satire is celebrating their 20th anniversary in the best of ways. According toScreen Rant,Comedy Central has announced an epic 8-day marathon ofSouth Parkas they count down the days to the debut of their 21st season.

With twenty years of episodes to choose from, fans will have plenty to keep their binge-watching session going. Comedy Central plans to air 127 hours ofSouth Park over a period of eight days, which adds up to 254 episodes. In case you forgot,The Simpsons did the same in 2014 to celebrate their 25th anniversary.

Comedy Central

TheSouth Parkmarathon begins on September 6 and will basically be a warm up for the new season which airs on September 13.

And of course, we can expect Comedy Central to inundate social media with news of the marathon using the newSouth Parkemoji on Twitter, along with the hashtags #SouthPark, #NewSouthPark, #SouthPark21, #Cartman, and #Memberberries (only real fans know what we're talking about).

The marathon will also be a great opportunity to revisit the best scenes from the show, from all the times Kenny died to the many hilarious Mr. Mackey quotes, mkay?

And if for some crazy reason you are new toSouth Park, the marathon will be an excellent opportunity for you to get to know the most politically incorrect cult show on television, even if the writers do say they are done making fun of Donald Trump...

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Racism in the spotlight – Youngstown Vindicator

Posted: at 3:36 am

Published: Fri, August 25, 2017 @ 12:00 a.m.

By Germine Awad

The Dallas Morning News

President Donald Trumps slowness to condemn the Charlottesville, Va., violence and subsequent comments that there was blame on both sides produced outrage, and rightly so.

Republican leaders such as Sens. Jeff Flake, Todd Young and Orrin Hatch condemned his excuse-making for white supremacists and the idea that the protesters and counter-protesters were morally equivalent. The fact that U.S. senators are commenting shows that people in power across political lines are actually talking about racism. That is a good thing.

Much of peoples horror regarding Trumps words comes from the notion that its obvious the president should condemn hate groups, and any show of support or sympathy is unacceptable.

Often, modern forms of racism, prejudice and discrimination are covert, hidden or implicit. It is not politically correct to openly communicate racist notions. Much of the discrimination that occurs is not explicit but rather subtle. For example, studies have shown that simply changing the name from a typically white-sounding name to a black-sounding name on otherwise identical resumes results in a 50 percent decrease in call-back interviews. In fact, there is overwhelming scientific evidence that subtle forms of discrimination exist and persist. However, people are uncomfortable talking about it or even acknowledging that racism could be a factor in areas such as the workplace, higher education, health care and schooling.

Bannons strategy

There is a tendency for people, especially politicians, to avoid topics such as discrimination and racism. Steve Bannon, who stepped down as White House chief strategist, recently said, The longer they (Democrats) talk about identity politics, I got em. I want them to talk about racism every day. If the left is focused on race and identity, and we go with economic nationalism, we can crush the Democrats.

Bannons comment suggests that talking about race and racism is such an unpleasant topic that he would have been able to achieve his political aims by not focusing on or acknowledging it.

Discomfort with racial topics partially stems from the notion that talking about race and racism is politically incorrect. People are so afraid of being called racist or saying something insensitive that they avoid the topic altogether. The covert nature of modern forms of prejudice may also make people reluctant to talk about it. Because these subtle forms of racism are not as obvious, it may be difficult for those who have not experienced or understood discrimination to acknowledge that it exists.

On the other hand, most Americans are comfortable condemning old-fashioned or overt forms of racism. For example, many Americans believe that neo-Nazis and other white supremacists are repugnant, and they arent afraid to voice that opinion.

We do, however, have real reasons to be concerned. The president has a great deal of power, and people turn to him for leadership. Although some have argued that Trump has failed as a leader in several practical ways, at the very least he is still the symbolic leader of our country. Trumps tepid response to the Charlottesville violence has invigorated white supremacists and spurred additional protests.

If we dont talk about racism, we cant begin to fix it.

Germine Awad is an associate professor of educational psychology at the University of Texas at Austin and is an affiliate of the department of African and African Diaspora studies. She wrote this for The Dallas Morning News

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Dolphins-Eagles Four Stars – The Intelligencer

Posted: at 3:36 am

Analyze this

In June, Jay Cutler was sharpening his television skills. The retired former Bears quarterback was all set to ease into a life of high-payed leisure. Then Dolphins starter Ryan Tannehill pulled up lame on a routine rollout during the earliest days of Miamis training camp. For showing that he can still fling it pretty good, give the formerly retired Cutler 3 stars

For years, Bill Belichick has advocated for giving coaches the ability to review any aspect of a play. Not that the Patriots head coach knows anything about football or anything, but its not such a crazy idea. The first quarter review that correctly gave the Dolphins the ball back at the 2 was going to be looked at no matter what because it was ruled a turnover. Still, wouldnt it be nice if a coach could review whatever he wanted? For putting unnecessary limits on how a challenge can be used, give the NFL 1 star

What comes after secondary? After Carson Wentz and Jay Cutler clinically dissected both teams defensive backfields in the first half, football fans had to wonder if two safeties, two corners and however many nickel players it will take can cover wide receivers in the second level. For making us consult the old Funk & Wagnalls dictionary to discover the word tertiary, give the defenses 1 star

In Baltimore, they have the Marching Ravens. Its a tradition started started when the Colts were still in town and Johnny Unitas and company ruled the NFL. In Washington, they have the leagues oldest marching band named in the same politically incorrect manner as the team itself and wearing culturally inappropriate uniforms that are even worse. The Eagles have the Drum Line. Baltimore and Washington got it right. Theres something primal about a 200-strong band playing at the football game. A dozen knuckleheads banging drums is sad in comparison. For being a pale comparison to real marching units, give the Silent-R drum line 1 star

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10+ Years of Activists Silenced: Internet Intermediaries’ Long History of Censorship – EFF

Posted: at 3:36 am

Recent decisions by technology companies, especially upstream infrastructure technology companies, to drop neo-Nazis as customers have captured public attentionand for good reason. The content being blocked is vile and horrific, there is growing concern about hate groups across the country, and the nation is focused on issues of racism and protest.

But this is a dangerous moment for Internet expression and the power of private platforms that host much of the speech on the Internet. People cheering for companies who have censored content in recent weeks may soon find the same tactic used against causes they love. We must be careful about what we are asking these companies to do and carefully review the processes they use to do it. A look at previous examples that EFF has handled in the past 10+ years can help demonstrate why we are so concerned.

This isnt just a slippery slope fear about potential future harm. Complaints to various kinds of intermediaries have been occurring for over a decade. Its clear that Internet technology companiesespecially those further upstream like domain name registrars are simply not equipped or competent to distinguish between good complaints and bad in the U.S. much less around the world. They also have no strong mechanisms for allowing due process or correcting mistakes. Instead they merely react to where the pressure is greatest or where their business interests lie.

Here are just a few cases EFF has handled or helped from the last decade where complaints went upstream to website hosts and DNS providers, impacting activist groups specifically. And this is not to mention the many times direct user platforms like Facebook and Twitter have censored content from artists, activists, and others.

Youll notice that complainers in these cases are powerful corporations. Thats not a coincidence. Large companies have the time, money, and scary lawyers to pressure intermediaries to do their biddingsomething smaller communities rarely have.

The story gets much more frightening when governments enter the conversation. All of the major technology companies publish transparency reports documenting the many efforts made by governments around the world to require the companies to take down their customers speech.[1]

China ties the domain name system to tracking systems and censorship. Russia-backed groups flag Ukrainian speech, Chinese groups flag Tibetan speech, Israeli groups flag Palestinian speech, just to name a few. Every state has some reason to try to bend the core intermediaries to their agenda, which is why EFF along with a number of international organizations created the Manila Principlesto set out the basic rules for intermediaries to follow when responding to these governmental pressures. Those concerned about the position of the current U.S. government with regard to Black Lives Matter, Antifa groups, and similar left-leaning communities should take note: efforts to urge the current U.S. government to treat them as hate groups have already begun.

Will the Internet remain a place where small, marginalized voices get heard? For every tech CEO now worried about neo-Nazis there are hundreds of decisions made to silence voices that are made outside of public scrutiny with no transparency into decision-making or easy ways to get mistakes corrected. We understand the impulse to cheer any decisions to stand up against horrific speech, but if we embrace upstream intermediary censorship, it may very well come back to haunt us.

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