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Global Psoriasis Treatment Market to Reach $12.8 Billion by 2025 … – Business Wire (press release)
Posted: June 29, 2017 at 10:45 am
DUBLIN--(BUSINESS WIRE)--Research and Markets has announced the addition of the "Global Psoriasis Treatment Market Size, Market Share, Application Analysis, Regional Outlook, Growth Trends, Key Players, Competitive Strategies and Forecasts, 2017 to 2025" report to their offering.
The Global Psoriasis Treatment Market was valued at US$ 7.9 Bn in 2016, and is expected to reach US$ 12.8 Bn by 2025, expanding at a CAGR of 5.4% from 2017 to 2025.
The psoriasis treatment market is rapidly growing due to factors such as growing prevalence in some countries, significant unmet needs, promising pipeline molecules would drive the growth of psoriasis market worldwide. For the purpose of study, global psoriasis treatment market is segmented on the basis of drug class such as TNF Inhibitors, Vitamin D analogues, interleukin blockers and other psoriasis medication. It is observed that, in the base year 2016, interleukin blockers was major revenue contributing segment due to its long-term safety with lower risk of infection and malignancy. Psoriasis treatment market is categorized on the basis of route of administration such as topical, oral and parenteral therapeutic drugs.
Currently, topical therapeutic drugs hold largest market share due to its safety, more effectiveness and targeted drug delivery. It is anticipated that parenteral therapeutic drugs would show significant growth during forecast period because newly approved biologics are generally preferred in moderate to severe psoriasis.
Companies Mentioned
Key Topics Covered:
Chapter 1 Preface
Chapter 2 Executive Summary
Chapter 3 Psoriasis Treatment Market Analysis
Chapter 4 Global Psoriasis Treatment Market, by Drug Class
Chapter 5 Global Psoriasis Treatment Market, by Route of Administration
Chapter 6 Global Psoriasis Treatment Market, by Geography
Chapter 7 Company Profiles
For more information about this report visit https://www.researchandmarkets.com/research/wnpcpw/global_psoriasis
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Global Psoriasis Treatment Market to Reach $12.8 Billion by 2025 ... - Business Wire (press release)
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Patients Who Tested Positive For Genetic Mutations Fear Bias … – NPR – NPR
Posted: at 10:44 am
Patients who underwent genetic screenings now fear that documentation of the results in their medical records could lead to problems if a new health law is enacted. Sam Edwards/Caiaimage/Getty Images hide caption
Patients who underwent genetic screenings now fear that documentation of the results in their medical records could lead to problems if a new health law is enacted.
Two years ago, Cheasanee Huette, a 20-year-old college student in Northern California, decided to find out if she was a carrier of the genetic mutation that gave rise to a disease that killed her mother. She took comfort in knowing that whatever the result, she'd be protected by the Affordable Care Act's guarantees of insurance coverage for pre-existing conditions.
Her results came back positive. Like her mother, she's a carrier of one of the mutations known as Lynch syndrome. The term refers to a cluster of mutations that can boost the risk of a wide range of cancers, particularly colon and rectal.
As Republican lawmakers advance proposals to overhaul the ACA's consumer protections, Huette frets that her future health coverage and employment options will be defined by that test.
She even wonders if documentation of the mutation in her medical records and related screenings could rule out individual insurance plans. She's currently covered under her father's policy. "Once I move to my own health care plan, I'm concerned about who is going to be willing to cover me, and how much will that cost," she says.
In recent years, doctors have urged patients to be screened for a variety of diseases and predisposition to illness, confident it would not affect their future insurability. Being predisposed to an illness such as carrying the BRCA gene mutations associated with breast and ovarian cancer does not mean a patient will come down with the illness. But knowing they could be at risk may allow patients to take steps to prevent its development.
Under the current health law, many screening tests for widespread conditions such as prediabetes are covered in full by insurance. The Centers for Disease Control and Prevention and the American Medical Association have urged primary care doctors to test patients at risk for prediabetes. But doctors, genetic counselors and patient advocacy groups now worry that people will shy away from testing as the ACA's future becomes more uncertain.
Dr. Kenneth Lin, a family physician at Georgetown University School of Medicine in Washington, D.C., says if the changes proposed by the GOP become law, "you can bet that I'll be even more reluctant to test patients or record the diagnosis of prediabetes in their charts." He thinks such a notation could mean hundreds of dollars a month more in premiums for individuals in some states under the new bill.
Huette says she's sharing her story publicly since her genetic mutation is already on her medical record.
But elsewhere, there have been "panicked expressions of concern," says Lisa Schlager of the patient advocacy group Facing Our Risk of Cancer Empowered (FORCE). "Somebody who had cancer even saying, 'I don't want my daughter to test now.' Or 'I'm going to be dropped from my insurance because I have the BRCA mutation.' There's a lot of fear."
Those fears, which come in an era of accelerating genetics-driven medicine, rest upon whether a gap that was closed by the ACA will be reopened. That remains unclear.
A law passed in 2008, the Genetic Information Nondiscrimination Act, bans health insurance discrimination if someone tests positive for a mutation. But that protection stops once the mutation causes "manifest disease" essentially, a diagnosable health condition.
That means "when you become symptomatic," although it's not clear how severe the symptoms must be to constitute having the disease, says Mark Rothstein, an attorney and bioethicist at the University of Louisville School of Medicine in Kentucky, who has written extensively about GINA.
The ACA, passed two years after GINA, closed that gap by barring health insurance discrimination based on pre-existing conditions, Rothstein says.
On paper, the legislation unveiled by Senate Majority Leader Mitch McConnell last week wouldn't let insurers set higher rates for people with pre-existing conditions, but it could effectively exclude such patients from coverage by allowing states to offer insurance plans that don't cover certain maladies, health analysts say. Meanwhile, the bill that passed the House last month does have a provision that allows states to waive protections for people with pre-existing conditions, if they have a gap in coverage of 63 days or longer in the prior year.
When members of a Lynch Syndrome social media group were asked for their views on genetic testing amid the current health care debate, about two dozen men and women responded. Nearly all said they were delaying action for themselves or suggesting that family members, particularly children, hold off.
Huette was the only one who agreed to speak for attribution. She says before the ACA was enacted, she witnessed the impact that fears about insurance coverage had on patients. Her mother, a veterinarian, had wanted to run her own practice but instead took a federal government job for the guarantee of health insurance. She died at the age of 57 of pancreatic cancer, one of six malignancies she had been diagnosed with over the years.
Huette says she doesn't regret getting tested. Without the result, Huette points out, how would she have persuaded a doctor to give her a colonoscopy in her 20s?
"Ultimately, my health is more important than my bank account," she says.
Kaiser Health News, a nonprofit health newsroom whose stories appear in news outlets nationwide, is an editorially independent part of the Kaiser Family Foundation.
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Patients Who Tested Positive For Genetic Mutations Fear Bias ... - NPR - NPR
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New colistin resistance gene identified in China – CIDRAP
Posted: at 10:44 am
Researchers in China have discovered another gene that confers resistance to the last-resort antibiotic colistin.
In a study yesterday in mBio, the researchers report that the MCR-3 gene was discovered in a fecal sample obtained from an apparently healthy pig at a farm in Shangdong province during a routine surveillance study of antimicrobial resistant bacteria. The gene was located on a colistin-resistant Escherichia coli isolate, on a plasmid that contained 18 additional antibiotic resistance genes.
The authors of the study say they're concerned the gene may already be widely disseminated, and that scientists should be on the lookout for it. "Screening for the mcr-3 gene should be urgently included in the surveillance of colistin-resistant Gram-negative pathogens from animals, humans, and the environment," they write.
The discovery was made by several members of the research team that first reported the discovery of the mobile colistin resistance gene MCR-1 in E coli from pigs, pork products, and humans in China in November 2015. That finding raised international concern, given that colistin is an antibiotic of last resort for multidrug-resistant bacterial infections. The gene's location on plasmids, which are highly mobile pieces of DNA that can be shared within and between different bacterial species, means that resistance to colistin can quickly spread.
Since then, MCR-1 has been identified in bacteria from humans, animals, and the environment in more than 30 countries, including the United States, and studies have documented the spread of the gene to the clinical setting in China. Earlier this year, Chinese scientists reported an outbreak of MCR-1carrying Klebsiella pneumoniae among patients in a pediatric leukemia ward.
In addition, six different variants of the MCR-1 gene have been reported, along with a second mobile resistance gene, MCR-2.
In yesterday's study, the researchers report that MCR-3 was identified when molecular testing showed the colistin-resistant E coli isolate was negative for both MCR-1 and MCR-2, but contained an unknown colistin resistance gene that could be transferred to another E coli strain. Further analysis revealed that the gene was located on a plasmid similar to MCR-1carrying plasmids.
The investigators also found that the genomic sequence of MCR-3 closely resembled sequences found in Enterobacteriaceae and Aeromonas bacteria collected from both clinical infection and environmental samples in 12 countries on four continents, a finding that suggests the previously unidentified gene may already have spread. "Due to the ubiquitous profile of aeromonads in the environment and the potential transfer of mcr-3 between Enterobacteriaceae and Aeromonas species, the wide spread of mcr-3 may be largely underestimated," they write.
Up until recently, colistin was widely used in Chinese agriculture, and MCR-1 is thought to be a product of selection pressure caused by that use. China banned use of the drug in animal feed in 2016, based in part on the discovery of MCR-1.
Because of its toxicity, colistin was rarely used in human medicine until the late 1990s, when resistance to other last-resort drugs, including carbapenems, necessitated its use in serious multidrug-resistant infections. Colistin is on the World Health Organization's list of critical antimicrobials for human medicine.
One of the major concerns about MCR-1 and its offshoots is that it's often located on plasmids that contain other antibiotic resistance genes. That raises the possibility of bacterial infections that will not respond to any antibiotic. The authors say continuous monitoring for mobile resistance elements in colistin-resistant bacteria is "imperative for understanding and tackling the dissemination of mcr genes in both the agricultural and health care sectors."
Scientists with the SENTRY Antimicrobial Surveillance Program, which monitors worldwide pathogens and changes in antibiotic resistance patterns, have been tracking the global spread of MCR-1 since it was identified, while the Centers for Disease Control and Prevention has been hunting for the gene in the United States.
See also:
Jun 27 mBio study
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The gene behind follicular lymphoma – Medical Xpress
Posted: at 10:44 am
June 28, 2017 Disruption of a region in chromosome 6 or epigenetic modifications of the DNA block Sestrin1 expression and these contribute to the development of follicular lymphoma. Credit: Elisa Oricchio/Natalya Katanayeva/EPFL
Follicular lymphoma is an incurable cancer that affects over 200,000 people worldwide every year. A form of non-Hodgkin lymphoma, follicular lymphoma develops when the body starts making abnormal B-cells, which are white blood cells that in normal conditions fight infections. This cancer is associated with several alterations of the cell's DNA, but it has been unclear which gene or genes are involved in its development. EPFL scientists have now analyzed the genomes of more than 200 patients with follicular lymphoma, and they discover that a gene, Sestrin1, is frequently missing or malfunctioning in FL patients. The discovery opens to new treatment options and it is now published in Science Translational Medicine.
One of the common features of follicular lymphoma is a genetic abnormality between two chromosomes (14 and 18). In an event known as "chromosomal translocation" the two chromosomes "swap" certain parts with each other. This triggers the activation of a gene that protects cells from dying, making cells virtually immortalthe hallmark of a tumor.
Moreover, approximately 30% of follicular lymphoma patients lose also a portion of chromosome 6, affecting multiple genes involved in suppressing the emergence of a tumor. These patients typically have poor prognosis. Another 20 % of patients have alterations causing chromosomal disorganization and the consequent malfunctioning of several genes and proteins. The bottom line is that for both group of patients it is very difficult to pinpoint which of all the affected genes are actually causing the disease.
The lab of Elisa Oricchio at EPFL, with colleagues from the US and Canada, analyzed the genomes of over 200 follicular lymphoma patients. Their analyses revealed that a specific gene, Sestrin1, can be harmed by both loss of chromosome 6 and silenced in patients.
Sestrin1 helps the cell defending itself against DNA damagefor example after exposure to radiationand oxidative stress. In fact, Sestrin1 is part of the cell's anti-tumor mechanism that stops potentially cancerous cells from growing.
Disruption of a region in chromosome 6 or epigenetic modifications of the DNA block Sestrin1 expression and these contribute to the development of Follicular Lymphoma.
Beyond identifying the Sestrin1 gene as frequently altered in FL patients, the scientists demonstrated that Sestrin1 is able to suppress tumors in vivo. They showed that Sestrin1 exerts its anti-tumor effects by blocking the activity of a protein complex called mTORC1, which is well known for controlling protein synthesis as well as acting as a sensor for nutrient or energy changes in the cell.
Finally, the identification of loss of Sestrin1 as a key event behind the development of follicular lymphoma is particular important because it helps identifying patients that will benefit from new therapies. Indeed, this study shows that the therapeutic efficacy of a new drug that is currently in clinical trial depends on Sestrin1. Importantly, this dependency can be extended beyond follicular lymphoma to other tumor types.
Explore further: Combination therapy may help patients with follicular lymphoma
More information: E. Oricchio el al., "Genetic and epigenetic inactivation of SESTRIN1 controls mTORC1 and response to EZH2 inhibition in follicular lymphoma," Science Translational Medicine (2017). stm.sciencemag.org/lookup/doi/10.1126/scitranslmed.aak9969
A new study in The Journal of Experimental Medicine reveals that a high-risk group of patients with follicular lymphoma could benefit from a novel drug combination.
Mutations present in a blood cancer known as follicular lymphoma have revealed new molecular targets for potential treatments, according to researchers at Queen Mary University of London (QMUL) together with collaborators ...
Immune cellular therapy is a promising new area of cancer treatment. Anti-cancer therapeutics, such as chimeric antigen receptor (CAR) modified T cells, can be engineered to target tumor-associated antigens to attack and ...
Follicular lymphoma (FL), the second most common form of non-Hodgkin lymphoma, is a largely incurable disease of B cells, yet in many cases, because of its indolent nature, survival can extend to well beyond 10 years following ...
The goal for many cancer patients is to reach the five-year, disease-free mark, but new research from UR Medicine's Wilmot Cancer Institute suggests that two years might be a more practical survival goal for people with follicular ...
(HealthDay)An initial watch-and-wait strategy does not have a detrimental effect on the freedom from treatment failure (FFTF) or overall survival rate in selected patients with low-tumor burden follicular lymphoma compared ...
While mutations in protein-coding genes have held the limelight in cancer genomics, those in the noncoding genome (home to the regulatory elements that control gene activity) may also have powerful roles in driving tumor ...
Scientists have had limited success at identifying specific inherited genes associated with prostate cancer, despite the fact that it is one of the most common non-skin cancers among men. Researchers at University of Utah ...
Cancerous tumors are formidable enemies, recruiting blood vessels to aid their voracious growth, damaging nearby tissues, and deploying numerous strategies to evade the body's defense systems. But even more malicious are ...
Follicular lymphoma is an incurable cancer that affects over 200,000 people worldwide every year. A form of non-Hodgkin lymphoma, follicular lymphoma develops when the body starts making abnormal B-cells, which are white ...
Leukemia researchers led by Dr. John Dick have traced the origins of relapse in acute myeloid leukemia (AML) to rare therapy-resistant leukemia stem cells that are already present at diagnosis and before chemotherapy begins.
Adding an investigational antibody to the chemotherapy rituximab appears to restore its cancer-killing properties in certain leukemia patients with a natural resistance to the drug, according to a small, proof-of-concept ...
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Researchers propose new approach to identify genetic mutations in men with prostate cancer – Medical Xpress
Posted: at 10:44 am
June 29, 2017 Micrograph showing prostatic acinar adenocarcinoma (the most common form of prostate cancer) Credit: Wikipedia
Scientists have had limited success at identifying specific inherited genes associated with prostate cancer, despite the fact that it is one of the most common non-skin cancers among men. Researchers at University of Utah Health studied prostate cancer patients with multiple cancer diagnoses, many who would not be recommended for genetic tests following current guidelines, to identify genetic mutations that may influence cancer treatment and cancer risk assessment for family members. Their findings are reported in the June issue of the journal Cancer.
"We commonly use a combination of a patient's personal and family cancer histories to identify those individuals who may have a mutation in a gene that predisposes that individual to developing cancers," said Patrick Pili, M.D., medical oncology fellow at the University of Texas MD Anderson Cancer Center. "Testing for hereditary cancers impacts not only the patient with cancer but also potentially the cancer screening and health outcomes of their entire family, but many prostate cancer patients do not meet the current guidelines to test for genetic cancer heritability."
Pili was part of a research team led by Kathleen Cooney, M.D., chair of the Department of Internal Medicine at U of U Health and a Huntsman Cancer Institute investigator, who proposed a strategy to identify germline mutations in men selected for the study based on their clinical history not their family history.
The study was highly selective, including 102 patients who had been diagnosed with prostate cancer and at least one additional primary cancer, like melanoma, pancreatic cancer, testicular cancer, or Hodgkin lymphoma.
The researchers examined the frequency of harmful germline mutations in this group of men. These mutations originate on either the egg or sperm and become incorporated into the DNA of every cell in the body of the resulting offspring.
Using next generation sequencing, the researchers found that 11 percent of the patients had a disease-causing mutation in at least one cancer-predisposing gene, which suggests these genetic variations contributed to their prostate cancer. Cooney found no difference in cancer aggressiveness or age of diagnosis compared to patients without these mutations.
In addition, a certified genetic counselor and co-investigator Elena Stoffel, M.D., University of Michigan Comprehensive Cancer Center, reviewed personal and family histories from each patient to determine whether they would meet clinical genetic testing guidelines. The majority of the men in the study, 64 percent, did not meet current criteria to test for hereditary cancer based on personal and/or family history.
The findings suggest that there are men with heritable prostate cancer-predisposing mutations that are not eligible for genetic screening under current guidelines.
"This is the first paper in which we can show the potential of using a clinical history of multiple cancers, including prostate cancer, in a single individual to identify inherited germline mutations," Cooney said.
The majority of harmful mutations identified were in genes involved in DNA repair.
"These mutations prevent the DNA from healing itself, which can lead to a predisposition for cancer," Cooney said.
This result is also beneficial because drugs like PARP [poly ADP ribose polymerase] inhibitors have a better success rate in treating cancers with the underlying gene mutation associated with DNA repair.
Cooney cautions that this is a small pilot study rather than a broader epidemiological survey, and it consists of a highly specific subset of patients.
"We cannot generalize these findings to the broader population, because we used highly selective criteria to tip us off to patients that may have mutations outside typical hereditary genetic patterns," she said.
The 102 patients included in the study were identified from the University of Michigan's Prostate Cancer Genetics Project, which registers patients who are diagnosed with prostate cancer before age 55 or who have a first- or second-degree relative with prostate cancer. In addition, the research team identified patients from the University of Michigan's Cancer Genetics Registry, which includes individuals with personal or family history suggestive of a hereditary risk of cancer.
"Our findings are in line with those of other studies, suggesting that approximately 1 in 10 men with advanced prostate cancer harbors a genetic variant associated with increased cancer risk," said Stoffel. "While family history is an important tool, there may be better ways to identify patients with genetic risk."
Future studies with larger sample sizes will include sequencing of tumors that will allow investigators to more carefully explore the different features associated with tumors that arise in individuals with germline mutations.
"This approach will help us identify patients at greater risk for aggressive prostate cancer so they can seek earlier screening while pre-symptomatic," Cooney said.
Explore further: Are men with a family history of prostate cancer eligible for active surveillance?
More information: Patrick G. Pili et al. Germline genetic variants in men with prostate cancer and one or more additional cancers, Cancer (2017). DOI: 10.1002/cncr.30817
Journal reference: Cancer
Provided by: University of Utah
Active surveillancecareful monitoring to determine if or when a cancer warrants treatmentis an increasingly prevalent choice for prostate cancer, but it's unclear if the strategy is appropriate for men with a family ...
Inherited mutations in genes that function to repair DNA may contribute to metastatic prostate cancer more than previously recognized, according to a study out today in the New England Journal of Medicine. Though infrequent ...
African-American men develop prostate cancer more often than other men, and it tends to be more deadly for this population. Some of the differences seem to be due to socioeconomic factors, but scientists wondered whether ...
(HealthDay)A man's risk of aggressive and fatal prostate cancer may be heavily influenced by gene mutations previously linked to breast and ovarian cancer in women, a trio of new studies suggests. Findings from the studies ...
Scientists are reporting a test which can predict which patients are most at risk from aggressive prostate cancer, and whether they suffer an increased chance of treatment failure. This test, reported at the European Association ...
While mutations in protein-coding genes have held the limelight in cancer genomics, those in the noncoding genome (home to the regulatory elements that control gene activity) may also have powerful roles in driving tumor ...
Scientists have had limited success at identifying specific inherited genes associated with prostate cancer, despite the fact that it is one of the most common non-skin cancers among men. Researchers at University of Utah ...
Cancerous tumors are formidable enemies, recruiting blood vessels to aid their voracious growth, damaging nearby tissues, and deploying numerous strategies to evade the body's defense systems. But even more malicious are ...
Follicular lymphoma is an incurable cancer that affects over 200,000 people worldwide every year. A form of non-Hodgkin lymphoma, follicular lymphoma develops when the body starts making abnormal B-cells, which are white ...
Leukemia researchers led by Dr. John Dick have traced the origins of relapse in acute myeloid leukemia (AML) to rare therapy-resistant leukemia stem cells that are already present at diagnosis and before chemotherapy begins.
Adding an investigational antibody to the chemotherapy rituximab appears to restore its cancer-killing properties in certain leukemia patients with a natural resistance to the drug, according to a small, proof-of-concept ...
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Posted in Gene Medicine
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Lynchings Wrong, Selective Outrage Equally Cringe Worthy – News18
Posted: at 10:44 am
Let us be clear that lynch narratives in India are never secular they are impassioned and lopsided either one way or the other. This is why the discussion on Jantar Mantar protests cannot be done in isolation as a purely people's movement - for it may have begun as one but it is not anymore.
The problem with the world we inhabit today is polarisation. The issue is either pro or anti. Black or white. National or anti national. Secular or Communal.
You cannot talk logic and debate in a sustained fashion today, for the fear of uttering or writing something which is 'politically incorrect' - a term ideologically defined and defended by a group of elites in this country. Unfortunately, it has become imperative to wear an ideological cloak even while discussing moral questions, either because you have to defend selective secularism or because you have to expose the selective ideological amnesia and dementia. In the process, one may want to be as balanced as a weighing scale projecting two sides of the arguments, but one has to often choose 'touchy', 'politically incorrect', 'untouchable' issues for articulation. Balance can come only when there is equal and equitable, responsible and balanced articulation of reasons for and condemnation of all cases of human rights' violation, violence, rapes and riots.
There is of course no doubt that lynchings are inhuman, unfit as a marker of any human civilisation. And because all lynchings are wrong, the reportage of Muslims being killed by Hindus and Hindus being killed by 'some' people, in case the killers are Muslims, is as communal and targeted as lynchings themselves. For far too long narratives of organised hatred against the majority by the elite intellectuals and English media editors' guild in India have been defining a skewed and dangerous idea of secularism in this country.
Not everyone in this nation has the luxury of such incisive and piercing verbal articulation against violence or selective outrage. But their inability to capacitate the building of a verbose written or spoken narrative cannot be an impediment in a socialist democracy to dismiss their actions by a group of an entitled and intellectually elite mob.
A reaction can be and must be pulled out and called out for its socially debilitating ramifications. But a silence to even address the action which facilitated the reaction is as much a part of the lynch mob herd mentality. Unless we accept this reality, the facade of looking for solutions is optimistic hypocrisy.
I was expecting the 'organic' outburst of 'collective' anger at Jantar Mantar to protest against the recent humiliation of a Meghalayan woman by a part of this same English speaking colonial and feudal elite that has no qualms in calling a PM candidate unfit for his tea selling background.
I was expecting a protest against the murder of two males in the household of Kerala CM's home village and the pattern of lynch mob in Kerala. I was expecting a strong protest against Muslim lynch mobs who have brutally raped and murdered women in Hojai and Marghareita in Assam.
But I was expecting too much from the media perhaps who focused on Jantar Mantar and gave prime time slots to articulate what some elite groups comprising of some same faces who have made protests their way of overstaying their interests in Delhi.
Having said what I have said, I reiterate, all lynchings are wrong, abhorrent, a blot on humanity. And similarly cringe worthy is selective outrage. More pathetic is Congress-Communists clandestine combine that spills over its jugalbandi in such opportunistic free loading in protests like these.
(The author is assistant editor, India Foundation Journal, and project head, northeast operations. Views expressed are personal)
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GUVNL vets proposals to take over imported-coal power plants – Moneycontrol.com
Posted: at 10:44 am
State-run Gujarat Urja Vikas Nigam Ltd (GUVNL) is evaluating proposals to take over majority stake in the imported coal-based power plants of Tata Power, Adani Power and Essar Power.
The three companies running imported coal-based plants in Mundra and Salaya were suffering losses due to disallowance of compensatory tariff to insulate these firms from higher coal prices in Indonesia due to change in regulation.
In a desperate measure, these companies had even offered GUVNL to take over majority stake in these power plants at a token consideration of Re 1 only.
There was a buzz that the Gujarat government had shown disinterest to take over these plants for a token consideration as it would be politically incorrect step in view of forthcoming assembly election in the state this year.
"These proposals are still under evaluation," a source in the GUVNL said.
Earlier on the issue, Power Minister Piyush Goyal said here was a lot of discussions about "what would happen to these plants and to the availability of low-cost power to some other states. Nothing has come out as yet".
"I had suggested that these imported coal-based plants may also look at technical solutions to try to use more domestic coal because under SHAKTI scheme we would soon come out with a policy which will allow imported coal-based plant to bid for domestic coal," he added.
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GUVNL vets proposals to take over imported-coal power plants - Moneycontrol.com
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Top Canadian Court Permits Worldwide Internet Censorship – EFF
Posted: at 10:44 am
A country has the right to prevent the worlds Internet users from accessing information, Canadas highest court ruled on Wednesday.
In a decision that has troubling implications for free expression online, the Supreme Court of Canada upheld a companys effort to force Google to de-list entire domains and websites from its search index, effectively making them invisible to everyone using Googles search engine
The case, Google v. Equustek, began when British Columbia-based Equustek Solutions accused Morgan Jack and others, known as the Datalink defendants, of selling counterfeit Equustek routers online. It claimed California-based Google facilitated access to the defendants sites. The defendants never appeared in court to challenge the claim, allowing default judgment against them, which meant Equustek effectively won without the court ever considering whether the claim was valid.
Although Google was not named in the lawsuit, it voluntarily took down specific URLs that directed users to the defendants products and ads under the local (Canadian) Google.ca domains. But Equustek wanted more, and the British Columbia Supreme Court ruled that Google had to delete the entire domain from its search results, including from all other domains such Google.com and Google.go.uk. The British Columbia Court of Appealupheldthe decision, and the Supreme Court of Canada decision followed the analysis of those courts.
EFF intervened in the case, explaining [.pdf] that such an injunction ran directly contrary to both the U.S. Constitution and statutory speech protections. Issuing an order that would cut off access to information for U.S. users would set a dangerous precedent for online speech. In essence, it would expand the power of any court in the world to edit the entire Internet, whether or not the targeted material or site is lawful in another country. That, we warned, is likely to result in a race to the bottom, as well-resourced individuals engage in international forum-shopping to impose the one countrys restrictive laws regarding free expression on the rest of the world.
The Supreme Court of Canada ignored those concerns. It ruled that because Google was subject to the jurisdiction of Canadian courts by virtue of its operations in Canada, courts in Canada had the authority to order Google to delete search results worldwide. The court further held that there was no inconvenience to Google in removing search results, and Google had not shown the injunction would offend any rights abroad.
Perhaps even worse, the court ruled that before Google can modify the order, it has to prove that the injunction violates the laws of another nation thus shifting the burdent of proof from the plaintiff to a non-party. An innocent third party to a lawsuit shouldnt have to shoulder the burden or proving whether an injunction violates the laws of another country. Although companies like Google may be able to afford such costs, many others will not, meaning many overbroad and unlawful orders may go unchallenged. Instead, once the issue has been raised at all, it should be the job of the party seeking the benefit of an order, such as Equustek, to establish that there is no such conflict. Moreover, numerous intervenors, including EFF, provided ample evidence of that conflicts in this case.
Beyond the flaws of the ruling itself, the courts decision will likely embolden other countries to try to enforce their own speech-restricting laws on the Internet, to the detriment of all users. As others have pointed out, its not difficult to see repressive regimes such as China or Iran use the ruling to order Google to de-index sites they object to, creating a worldwide hecklers veto.
The ruling largely sidesteps the question of whether such a global order would violate foreign law or intrude on Internet users free speech rights. Instead, the court focused on whether or not Google, as a private actor, could legally choose to take down speech and whether that would violate foreign law. This framing results in Google being ordered to remove speech under Canadian law even if no court in the United States could issue a similar order.
The Equustek decision is part of a troubling trend around the world of courts and other governmental bodies ordering that content be removed from the entirety of the Internet, not just in that country's locale. On the same day the Supreme Court of Canadas decision issued, a court in Europe heard arguments as to whether to expand the right-to-be-forgotten worldwide.
EFF was represented at the Supreme Court of Canada and the British Columbia Court of Appeal by David Wotherspoon of MacPherson Leslie & Tyerman and Daniel Byma of Fasken Martineau DuMoulin.
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Top Canadian Court Permits Worldwide Internet Censorship - EFF
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Facebook: Too Big to Delete – WIRED
Posted: at 10:44 am
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g GOUv LK &(O5-)}*}s+?]OG+l|Ckw6yl6,h=;}UZBO]Kj:2{W{s[z~6N>*;K=?&-[pd~Y*o0*SaE~r(na5)&GQ[rcqeoF5R8{vYvFrzX3 IK j$_v?WF]$g7 RY|A}yP)o3z4s Kt ^{OXTj hyG_srr|;+9??OXs0...^>?i`n@r3wj/}0wEW!8+kr '#} K0(G-|[o_=HppgW9=9>-4'BOmWqf_jd+~j}>Md1fdOGBD#I 73VR19ZF&(}i1k!7dSy*b: Om]`ezn/_mjE8XW12)@4.PA(] 8 O![%GH*[cmzb*]?~TceQtLUW`)X!]@. sX3whu-3!J)CPsy g8jE$+)?YxSi7B{.k"1$?FV"1:[Rtn@d+~$Y1@@+G8"w;?WT,KRug1>hx~|6'? 4I>C _dw_!Zb+79TUK]~nI.FJM`z9'GpvXHD+mv(O.u*M}~D$,.TAmZel 2Z)t+m0D@s15p7U!+kj}|}TUa=OI]5uS1*d,LLNM]'jCR.f|{")1$] @ l/J_Oj)5Eu-L%r^0>|]yCZw{D%vzF hwv!ul;/pV,XamVB%'x1^]obwn6A
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Facebook: Too Big to Delete - WIRED
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Tucker Carlson Spotlights Twitter Censorship of Pro-Life Group – Church Militant
Posted: at 10:44 am
DETROIT (ChurchMilitant.com) - Twitter, a privately owned social media giant that boasts of more than 300 million users, is censoring a pro-life group's ads, labeling them hate speech.
On Monday, Tucker Carlson covered this ongoing censorship by Twitter on his show Tucker Carlson Tonight. Live Action is the pro-life group, who's ads are being called hate speech by Twitter and flagged on their social media platform.
Carlson invited on his show Catholic convert Lila Rose, founder and president of the organization, to discuss the issue. On the show, Rose explained exactly what Twitter was objecting to. "The kind of tweets," said Rose, "that they're calling a violation of their hate and sensitive policy show ultrasound images, they're fact checks of Planned Parenthood, they're discussing the prenatal life in its beauty. These are the sorts of tweets that Twitter is trying to block."
Carlson posted a picture of one such ad that Twitter refused to allow on its platform. It was a picture of a baby in utero with the caption, "I AM NOT A POTENTIAL HUMAN. I AM A HUMAN WITH POTENTIAL." On top of the ad is a message by Rose, which reads, "Everyone deserves the right to life! Join me in standing up for human dignity and the least of these."
According to Carlson, Twitter wants Live Action to delete these so-called "sensitive ads" before it will allow the group to buy more ads. Rose points out that Planned Parenthood (PP), the nation's biggest abortion chain, is allowed by Twitter to run ads on their platform, but Live Action, who she calls "the leading pro-life platform for the pro-life movement," is not allowed to do so. She says Twitter is claiming such ads violate their "hate and sensitive policy."
"This is something that they've been kind of keeping a secret, and now we're trying to get this news out that they've been blocking us," said Rose. Carlson responded, "But meanwhile the abortion industry gets to advertise all it wants."
Rose points out that the abortion giant PP has more than a one billion dollar budget and is committing almost 900 abortion every day, yet Twitter ironically says "they're not violating the hate and sensitive policy." She said Live Action is simply "exposing them, talking about the value of preborn life," which she says are messages that a lot of Americans agree with.
She says Twitter has been banning their ads for months now. She relates that Twitter wants them to delete their entire website and create an entirely new website before they can do any more advertising on Twitter. Carlson posted a response from Twitter, which claimed its policy was a set of "clear, transparent rules." Rose denies that the rules are clear because it "took over a year to finally get from Twitter what's wrong with these tweets showing ultrasounds."
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Tucker Carlson Spotlights Twitter Censorship of Pro-Life Group - Church Militant
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