Hello folks,
Most weekends this blog offers up a few substantial links to relevant HCV information, research and education, click here for previous "Weekend Reading" articles.
This weekend I am especially excited to point readers to the new "2012 Pipeline Report" by HIV i-Base and TAG.
Officially, The International AIDS Conference taking place in Washington, D.C. begins tomorrow, and runs through July 27. Over the next few weeks the public will have the opportunity to read daily highlights and press releases available at the conference website.
However, today in Washington HIV i-Base (U.K.) and Treatment Action Group (TAG) (U.S.) released the comprehensive - 2012 Pipeline Report, authors Polly Clayden, Simon Collins, Colleen Daniels, Nathan Geffen, Mark Harrington, Richard Jefferys, Coco Jervis, Karyn Kaplan, Erica Lessem, Tracy Swan; report on drugs in development and preventive technologies for HIV, hepatitis C (HCV), and Tuberculosis (TB).
The report is ready to view at the new website launched today by "TAG".
In the US, patient advocacy groups like TAG, continue to be the critical component in the fight against HIV, HCV and TB. I want to express my gratitude for the many years of pipeline reports, fact sheets, clinical trial guides, research, and advocacy that Tag has provided us with.
The press release from HIV i-Base and Tag discussing the new report is listed below, along with links to all the invaluable information.
For the HCV community, there is a particular article written by Tracy Swan and Karyn Kaplan you won't want to miss; Hepatitis C Drug Development Goes from Pony Ride to Rocket Launch.
The in depth report includes some of the following topics; HCV drug resistance, DAA drug-drug interactions, nucleosides and nucleotide polymerase inhibitors, HCV protease inhibitors, the next generation of drugs, HCV quad therapy, SVR-4 ,SVR-12, interferon free therapy, ABT-450/r, ACH-1625, BI 201335, BMS-650032, BMS-790052, danoprevir, genotypes 1-4, GS-7977 formally/PSI-7977, GS-9256, lambda, MK-7009, TMC435 and much more....
Links:
The 2012 Pipeline Report: HIV, Hepatitis C Virus (HCV), and Tuberculosis (TB) Drugs, Diagnostics, Vaccines, and Preventive Technologies in Development by Polly Clayden, Simon Collins, Colleen Daniels, Nathan Geffen, Mark Harrington, Richard Jefferys, Coco Jervis, Karyn Kaplan, Erica Lessem, and Tracy Swan is available online at:
Most weekends this blog offers up a few substantial links to relevant HCV information, research and education, click here for previous "Weekend Reading" articles.
This weekend I am especially excited to point readers to the new "2012 Pipeline Report" by HIV i-Base and TAG.
Officially, The International AIDS Conference taking place in Washington, D.C. begins tomorrow, and runs through July 27. Over the next few weeks the public will have the opportunity to read daily highlights and press releases available at the conference website.
However, today in Washington HIV i-Base (U.K.) and Treatment Action Group (TAG) (U.S.) released the comprehensive - 2012 Pipeline Report, authors Polly Clayden, Simon Collins, Colleen Daniels, Nathan Geffen, Mark Harrington, Richard Jefferys, Coco Jervis, Karyn Kaplan, Erica Lessem, Tracy Swan; report on drugs in development and preventive technologies for HIV, hepatitis C (HCV), and Tuberculosis (TB).
The report is ready to view at the new website launched today by "TAG".
In the US, patient advocacy groups like TAG, continue to be the critical component in the fight against HIV, HCV and TB. I want to express my gratitude for the many years of pipeline reports, fact sheets, clinical trial guides, research, and advocacy that Tag has provided us with.
The press release from HIV i-Base and Tag discussing the new report is listed below, along with links to all the invaluable information.
For the HCV community, there is a particular article written by Tracy Swan and Karyn Kaplan you won't want to miss; Hepatitis C Drug Development Goes from Pony Ride to Rocket Launch.
The in depth report includes some of the following topics; HCV drug resistance, DAA drug-drug interactions, nucleosides and nucleotide polymerase inhibitors, HCV protease inhibitors, the next generation of drugs, HCV quad therapy, SVR-4 ,SVR-12, interferon free therapy, ABT-450/r, ACH-1625, BI 201335, BMS-650032, BMS-790052, danoprevir, genotypes 1-4, GS-7977 formally/PSI-7977, GS-9256, lambda, MK-7009, TMC435 and much more....
Links:
The 2012 Pipeline Report: HIV, Hepatitis C Virus (HCV), and Tuberculosis (TB) Drugs, Diagnostics, Vaccines, and Preventive Technologies in Development by Polly Clayden, Simon Collins, Colleen Daniels, Nathan Geffen, Mark Harrington, Richard Jefferys, Coco Jervis, Karyn Kaplan, Erica Lessem, and Tracy Swan is available online at:
and as an interactive web report at:
Press Release:
HIV i-Base/Treatment Action Group 2012 Pipeline Report Reveals
Deep Gaps between Scientific Promise and Program Delivery
– Recent Advances in Biomedical HIV, Hepatitis C Virus (HCV), and Tuberculosis (TB) Prevention and Treatment Are Not Reaching Those Who Need Them Most –
– Political Leaders Continue to Break Domestic, Global Health Commitments –
Pointing to the recent dramatic demonstration that earlier anti-HIV therapy can reduce transmission of the virus by 96% among stable sexual partners with differing HIV status, Clayden and Harrington comment, “Three papers published in the past year provide the scientific, public health, and policy framework for accelerating the response to the HIV pandemic such that within a few years the spread of HIV can be reversed, saving millions of lives and billions of dollars, using existing antiretroviral therapy earlier and more broadly around the world. The only thing holding us back is the lack of economic and political leadership at the highest levels.”
The authors point out that while 7 million people are receiving lifesaving HIV treatment, the new scientific results indicate that up to 27 million more will need such therapy to realize the promise of earlier treatment for both individuals and public health. More preliminary results also suggest that targeting HIV prophylaxis for high-risk HIV-negative individuals can also prevent transmission, when administered in well-organized and comprehensive prevention programs, as indicated by the U.S. Food and Drug Administration (FDA) approval, earlier this month, of the first two-drug combination licensed for HIV prevention. Still more preliminarily, a single patient, Timothy Brown, has been cured of HIV infection after receiving an immune system transplant with stem cells genetically resistant to HIV. Brown has remained off HIV treatment for more than five years with no ongoing HIV replication detected.
There are many promising new HIV therapy candidates in the pipeline, as indicated in Simon Collins’s article on adult antiretrovirals, with at least 15 new drugs and combinations in phase II and III studies. In her article on the pediatric HIV pipeline, Polly Clayden demonstrates that some sponsors have made significant progress in more rapidly developing new drug options for children living with HIV. “Accelerating the regulatory approval gap between rich countries and poor ones, and between adult HIV approvals and pediatric availability, is one of the most important recommendations in this year’s Pipeline,” commented Clayden. “Children and people in developing countries should be given the best chance for durable responses to therapy, with 21st-century drugs, not forced to take second-class, toxic, and inferior drugs from the 1990s just because they are cheaper or were developed first.”
Nathan Geffen of South Africa’s Treatment Action Campaign (TAC) emphasizes the many years that can elapse needlessly between approval of new HIV drugs in Europe and America and their availability in countries such as South Africa, which has both the world’s largest HIV epidemic and its largest HIV treatment program. He points out that regulatory inefficiency by South Africa’s Medicines Control Council (the country’s equivalent of the FDA) delays both the opening of critical clinical trials and the approval of safer and more effective new drugs.
Richard Jefferys covers this year’s groundbreaking FDA review of Truvada for preexposure HIV prophylaxis (PrEP), HIV cure research, and the ongoing struggle to discover and develop safe and effective vaccines to prevent HIV transmission. For the first time in three decades, there are concrete indications that progress is at hand in biomedical HIV prevention, vaccination, and cure.
Moving to the hepatitis C virus (HCV) pandemic, which affects over 160 million people worldwide and is the leading cause of death among people with HIV in America and Europe, Tracy Swan and Karyn Kaplan provide a sweeping overview of the explosive developments in HCV combination therapy and cure, with over 25 direct-acting antivirals (DAAs) in development for HCV. Last year’s regulatory approvals of the first two protease inhibitors to treat HCV marked the cutting edge of a tidal wave of new DAAs, oral treatments for HCV that can cure more cases than ever before, sometimes without the former therapy backbone of peginterferon alfa, which is both expensive (over US$20,000/year) and highly toxic. The HCV DAA revolution makes it possible for the first time to envisage eradication of HCV—which has no natural animal hosts, and can be cured in some cases in just a few months with two or three DAAs—in the coming two decades. Swan and Kaplan caution that currently infrastructure and reimbursement mechanisms to cover treatment and care costs for people with HCV are lacking almost everywhere, and must be rapidly expanded to treat and cure the millions who are living with HCV.
Tuberculosis research has undergone a renaissance, particularly in TB drugs and regimens, but hardly a revolution (unlike HCV). Erica Lessem shows significant progress in new TB drug and regimen development, with two new drugs—bedaquiline from Janssen and delamanid from Otsuka—being filed with regulators for accelerated approval to treat drug-resistant forms of TB; the first two novel combination studies in decades having been started by the TB Alliance; and a two-drug, twelve-dose, curative regimen newly recommended by the U.S. government for prevention of latent TB infection (LTBI). As slow progress in TB diagnostics and vaccine research reveals, investment in TB research is far too low to permit rapid progress.
“We call on political leaders worldwide to step up implementation of new scientific discoveries to bridge the global and domestic prevention and treatment gaps,” concluded Clayden and Harrington.
# # #
http://www.treatmentactiongroup.org/pipeline-report/2012
and as an interactive web report at:
http://www.pipelinereport.org.
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