Showing posts with label vaccination. Show all posts
Showing posts with label vaccination. Show all posts

Sunday, October 3, 2010

CNS coverage from 2nd Global Forum on Tuberculosis (TB) Vaccines, Tallinn, Estonia

Babs Verblackt wrote on issues around the tuberculosis (TB) vaccines, on-site from the 2nd Global Forum on TB Vaccines, in Tallinn, Estonia (21-24 September 2010). Babs is freelance journalist, a Fellow of CNS Writers' Bureau and Associate Communications at TuBerculosis Vaccine InitiativeTBVI). Read more



These CNS articles were published in a diverse range of media outlets of many countries including: India, Pakistan, Thailand, Sri Lanka, Nepal, Brunei Darussalam, Ghana, United Arab Emirates (UAE), USA, New Zealand, Bangladesh, South Korea, among others. CNS also used social media extensively to disseminate articles through Twitter (3000+), Facebook (2600+), younews, reddit, Google Buzz, Digg, newstrust, HealthDev.net, AIDSspace, nowpublic and others. These articles were also disseminated via electronic discussion forums on specific issues like SEA-AIDS, Stop-TB, Lung Health, to name a few. Synopsis of these articles was translated in Thai language and broadcasted through FM 102.5 in Thailand.

Five CNS articles written by Babs Verblackt, from the 2nd Global Forum for TB Vaccines are as follows:

Thanks

Thursday, September 30, 2010

Clinical trial capacity remains challenge for TB vaccine development

Tallinn, Estonia: While progress is being made in the development of new vaccines against tuberculosis (TB), sufficient clinical trial capacity remains a major challenge, researchers reaffirmed at the Second Global Forum on TB Vaccines in Tallinn, Estonia (21-24 September 2010). Read more



Scientists from around the world presented the latest developments in their research on new TB vaccines. Eight vaccine candidates were presented, which are now all tested on humans in various stages of clinical trials, many in Africa. Currently the most advanced vaccine candidate is the MVA85A vaccine developed by Oxford University.

While the current TB vaccine candidates have shown promising early-stage results on safety and immunogenicity in studies conducted at well-established world class TB vaccine research sites, further tests are required and additional clinical trial sites will be needed to meet the demand. The already long and complicated process of testing vaccines is made more challenging by a general lack of capacity for clinical trials worldwide, the researchers acknowledged.

"It is important to involve local communities from the very beginning," stressed Dr Tom Evans, MD, Chief Scientific Officer at Aeras Global TB Vaccine Foundation in a presentation.

Evans mentioned the need to address language issues, local (traditional) medical practices, local perceptions about giving blood and participating in clinical trials as necessary steps needed to avoid possible pitfalls. But even logistical problems such as power grid problems and limited access to electronic data, or unexpected situations such as worldwide travel problems and instability of governments can influence the course of clinical trials.

According to Robert Nakibumba, Community Representative to the New Vaccines Working Group at Stop TB Partnership, creating 'minds for a new TB vaccine' on community level is a challenge as well. "Many people think: there is a TB vaccine already, why you come up with a new vaccine?" he said in a later session at the meeting. "We have to tactfully explain to the community the limitations of BCG, they must know the existing tool is not effective."

BCG (Bacille Calmette Guérin) is the only currently available vaccine against TB. It is widely used around the globe and protective against severe forms of TB in children. But it is not effective enough against pulmonary TB in adolescents and adults, the most common and most infective form of TB worldwide.

Nakibumba also underlined the importance of involving local communities. "They are not only patients or participants in clinical trials. They are going to get the vaccine, they are serious stakeholders."

The Second Global Forum on TB Vaccines in Tallinn, Estonia, last week brought together around 200 scientists, clinicians, manufacturers, NGOs and governmental institutions from around the world. They reviewed the progress made in vaccine development in the past decade and look forward to the challenges and opportunities ahead.


Babs Verblackt - CNS
(The author is a freelance journalist, a Fellow of CNS Writers' Bureau and Associate Communications at TuBerculosis Vaccine InitiativeTBVI


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Wednesday, September 22, 2010

TB doesn't get the prioritization it needs

Tallinn, Estonia: Tuberculosis (TB) is considered a major public health issue by decision makers, yet commonly doesn't get the place of importance it needs as a health care priority. These are the preliminary results of a study presented at the Second Global Forum on TB Vaccines in Tallinn, Estonia, on Wednesday, 22 September 2010. Read more



The market research study provides an overview of national-level decision makers’ views on the introduction of new vaccines against TB. Undertaken in eight countries with high TB burdens, researchers conducted 86 one-on-one interviews (45-60 minutes) with senior Ministry of Health (MoH) civil servants responsible for vaccine introduction, MoH technical experts involved in delivering vaccines through the Expanded Programme on Immunization, senior Ministry of Finance (MoF) civil servants responsible for health budgets, senior public health clinicians, (children’s) health related NGOs, parliamentarians, and senior journalists. The study was conducted in China, India, South-Africa, Brazil, Russia, Mozambique, Cambodia and Romania.

The interviewees were presented with three hypothetical scenarios for new TB vaccines and asked questions about, among others, the likely demand and likelihood of rapid implementation. Overall, there was enthusiasm for (the use of) a new TB vaccine. "We still need to further analyze and break down the results, but generally they are encouraging," said Lew Barker, Senior Medical Advisor with the Aeras Global TB Vaccine Foundation. "What is striking is that the answers varied both within and between countries, ranging from positive to negative, and often with a wait and see attitude."

When the interviewees were initially asked about their country's major public healthcare priorities, none mentioned TB. Rather issues such as primary healthcare, mother and childcare, chronic diseases and HIV/AIDS topped the lists. "But if they were then asked about TB, the respondents immediately acknowledged it is a big problem that doesn't get the attention it deserves," Barker explained. "So TB is not at the top of their mind but it definitely is there on a lower level. It is a neglected disease - we already know that - that is one of the challenges the fight against TB has to face."

The results further showed a widespread dissatisfaction with the only currently available vaccine, Bacille Calmette Guérin (BCG). The vaccine is protective against severe forms of TB in children, but not effective enough against lung TB in adolescents and adults, the most common and most infective form of TB worldwide.

The market research study titled 'Barriers and Drivers for Introduction of New TB Vaccines' was done as part of a broader initiative of the Stop TB Partnership's Task Force on Economics and Product Profiles for New TB Vaccines. It will be published online later this year.

At the international conference in Tallinn, around 200 scientists, clinicians, manufacturers, NGOs and governmental institutions from around the world this week (September 21-24) review the progress made in vaccine development in the past decade and look forward to the challenges and opportunities ahead.

Babs Verblackt-CNS
(The author is a freelance journalist, a Fellow of CNS Writers' Bureau and Associate Communications at TuBerculosis Vaccine InitiativeTBVI


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Now Public News, India 
Topix News, Tallinn, Estonia  
New Zim Situation, Zimbabwe 
One News Page, Tallinn, Estonia
Tuberculosis Vaccine Initiatives (TBVI)
Bihar and Jharkhand News Service (BJNS)
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Monday, August 23, 2010

Rural child health initiative reaches out to UP's poor

Photo credit: Kulsum Mustafa
Wednesday and Saturdays are Routine Immunization days in Uttar Pradesh. From morning one witness rural women with infants in arms making a beeline for primary health centres. But June and December are more special months for little children in India's most populous state with very poor development indicators. It is in these two months when health call beacons all the under five in remotest corners of the state. Read more




"Bal Swasthya Poshan Mah" (BSPM) is a bi-annual government health programme that addresses the grave issue of malnutrition from which a major number of the state children suffer. During BSPM children are given the vital vitamin A dose the deficiency of which can result in preventable blindness.  The children also get the routine immunization (RI). During BSPM counseling of young mothers, pregnant and lactating women is also done regarding the right nutrition for their children which includes breastfeeding, complimentary feeding, supplementary feeding, usage of iodine salt, and proper sanitation.

While this health initiative is for all the 72 districts of Uttar Pradesh, special focus is being given on 15 districts which have been identified as 'high risk (HR).'

Farrukhabad, situated some 250 km from the state capital Lucknow is one such HR districts. The UP government has taken the help of UNICEF for this.

"The high risk district generally have a high density of Muslims and lower castes, the idea is to reach out to them and ensure that they are not left out in this health campaign," explained UNICEF medical representative Dr Deepak Sinha in the district.

"Kamaalganj, one of the six blocks in Farukkabad district has 50 per cent Muslim population. Thus efforts have been made to reach out to them through the leading Muslim persons in the area," he explained. Dr Tausif Baig, district coordinator, Farukkahabad, Social Mobilizing network, UNICEF said that they are going from door-to-door with a team to explain to the population the advantages of availing of the facilities during the BSPM.

He informed that their initiative of getting the publicity material printed in Urdu has got a lot of good response.

The team is also ensuring that reach out to the minority community during the weekly Friday congregations.

One can only hope that concentrated and sustained efforts will bear fruit and the community comes forward to avail of the health facilities being offered free of cost to them like to people of other community.

Kulsum Mustafa
(The author is a senior journalist and also the Secretary of Media Nest


Published in:
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Elites TV News, USA
Thai-Indian News, Bangkok, Thailand
Bihar and Jharkhand News Service (BJNS), Bihar /Jharkhand
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Thursday, July 15, 2010

Turning the Page to a New Era in HIV Prevention Research

AVAC Report warns promising developments in biomedical HIV prevention could be undermined by current conditions of the global AIDS response 

A new report from AVAC surveys the state of biomedical HIV prevention research, including the first evidence of vaccine-induced protection in humans and the emergence of ARV-based prevention—and provides strategic recommendations for moving forward in a time of constrained resources and faltering commitment to ending AIDS. Turning the Page, AVAC’s 13th annual report on the state of the HIV prevention research field, offers unique context and a timely critique for issues that will be center stage at the upcoming XVIII International AIDS  Conference (IAC) in Vienna, Austria. These issues are also central to the AIDS response outlined in the first ever US National HIV/AIDS Strategy, released on 13th of July 2010. Read more




As the report describes, scientific developments in several arenas of biomedical prevention research have re-energized the search for additional strategies. In the vaccine field this includes the first evidence of vaccine-induced protection and strides in identification of new potent, HIV-specific neutralizing antibodies. Antiretroviral-based prevention also shows potential, and the report provides context for the upcoming results of the CAPRISA 004 microbicide trial, the first effectiveness trial of an ARV-based prevention strategy in HIV-negative people.

The biomedical prevention research field must now develop strategies for pursuing new scientific leads and following through on promising developments without the guarantee of expanded financial resources. In addition, the implications of recent breakthroughs need to be explained clearly to diverse audiences. As the report describes, the next phase of human clinical trials will involve complex designs and questions, and their success will depend on the support of all stakeholder groups. It will be difficult to execute this ambitious research agenda in the context of fiscal constraint—and the field needs to address this head on.

“We face yawning gaps in funding for proven prevention and treatment and a crisis in financial and political will,” said Mitchell Warren, AVAC Executive Director. “There is skepticism about whether disease-specific funding for AIDS is cost effective and skepticism about whether limited funds for AIDS should include funding for AIDS prevention research.”

“The recent report from UNAIDS that proven HIV prevention is having a demonstrable impact on the epidemic in many African countries is good news. But to really have an impact on the epidemic we need additional funding and political commitments for AIDS treatment and prevention programs AND more funding for HIV prevention research,” Warren added.

“The AVAC Report makes the critical point that to capitalize on recent breakthroughs in HIV prevention, we must find smart and innovative ways to make the best use of available funding,” said Chris Collins, AVAC Board Member and Vice President and Director, Public Policy at amfAR, The Foundation for AIDS Research.

The HIV prevention research field has been buoyed by major breakthroughs in recent months and Turning the Page calls for researchers, funders and others to prioritize collaboration and nimble and adaptive planning for replenishing the pipeline with new products and designing clinical trials that will yield the most information to move the field forward.

In recent years, the HIV prevention research agenda has broadened beyond vaccines and microbicides to include antiretroviral-based prevention, including pre-exposure prophylaxis, and, more recently, efforts to understand the role of treatment as prevention. At the same time, HIV treatment programs—once thought to be impossible to implement in developing countries—have expanded to reach millions of people around the world.

“The HIV prevention research agenda must take into account the new realities of the fight against AIDS. We believe that new prevention programs cannot be built while current treatment programs are faltering,” Warren said. “To reach the goal of universal access to healthcare—which includes comprehensive AIDS treatment and prevention—advocates, researchers, health care providers, funders and policy makers must speak with one voice.”

Turning the Page lays out the critical components of a response to AIDS that unites treatment and prevention, including:

* Sustain and expand current treatment and care programs: Funding restrictions are beginning to take a damaging toll on AIDS treatment programs at the precise moment that data are emerging to show that ARV treatment prevents deaths, lowers health care costs and can reduce the risk of HIV transmission. Donors and policy makers must take the critical steps needed to forestall further damage and put treatment programs back on track.

* Actively explore treatment as prevention: There is compelling evidence that earlier initiation of antiretrovirals in HIV-positive people can reduce the risk that they will infect sexual partners with HIV. Additional data will come from an ongoing clinical trial, but the world should begin exploring the practical approaches and implications of scaling up HIV treatment as prevention that can help guide policy makers’ decision-making about potential introduction of treatment as prevention when the data become available.

* Plan for ARV-based prevention: Neither oral PrEP nor topical ARV-based microbicides have yet been proven to have benefit. But, if they do, they will need to be delivered strategically, in programs that provide clear, integrated messages about the risks and benefits of ARVs for prevention in HIV-negative people. Results from CAPRISA 004, the first ARV-based microbicide effectiveness trial, will be delivered next week at AIDS 2010 and results from initial PrEP effectiveness trials are expected in the next 12 months. The field needs to be prepared to address the many questions that will emerge from these results and develop rational plans for ensuring the best use of the potential new options.

“We must also be ready to be surprised. The greatest advances in the fight against AIDS have come about because people and institutions refused to accept conventional wisdom about what was possible,” Warren said. “In 15 years of advocating for AIDS vaccines, we at AVAC have witnessed many moments when an AIDS vaccine was deemed a scientific impossibility. Yet, a trial that had been all but discounted by many provided evidence that a preventive AIDS vaccine is possible. And AIDS treatment programs and their clients have flourished in every possible context around the globe in the face of those who said it was impossible.”

“Now is the best time to invest in an expanded response to the AIDS epidemic. AVAC stands with the global community of advocates for HIV prevention, treatment, research and implementation to expect and demand an extraordinary response to this unprecedented epidemic—our only hope of closing the book on AIDS,” Warren added.

Turning the Page and other AVAC publications, including an upcoming report on anticipating the results of ARV-based prevention trials are available online at www.avac.org 


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Thursday, July 1, 2010

James Connolly Committed to Accelerating the Development of New Vaccines to Prevent TB

Aeras(TM)The Aeras Global TB Vaccine Foundation today announced that James E. Connolly has been named President and Chief Executive Officer. He joins Aeras after a career in the pharmaceutical industry, most recently as Executive Vice President and General Manager of Wyeth Vaccines. He will take over as Aeras President and CEO on August 9, 2010. Read more



"As Aeras continues its momentum to develop new tuberculosis vaccines for all who need them, we are delighted that Jim Connolly will lead the organization through its next phase," said R. Gordon Douglas, Jr., MD, the Executive Chairman of the Aeras Global TB Vaccine Foundation. "Jim has exactly the right mix of leadership and passion for Aeras' important, lifesaving mission. His management and financial expertise and his vaccine experience will be tremendous assets to Aeras as it advances its portfolio of TB vaccine candidates through late-stage trials and ultimately licensure and distribution." Dr. Douglas added that Jim Connolly's background, which includes efforts to expand access to vaccines in developing countries, will be valuable in working with Aeras' broad array of partners worldwide.

"Leading Aeras provides an exciting opportunity to apply all that I have learned during more than twenty years in the pharmaceutical industry to one of the world's most pressing challenges: freeing the world of tuberculosis, which continues to kill almost two million people each year," said Jim Connolly. "I look forward to working with the many dedicated and gifted vaccine experts at Aeras and its numerous research and development partners around the world."

At Aeras, a non-profit product development partnership, Jim Connolly will lead a team of over 140 employees working to discover, develop and deliver safer, more effective and affordable new vaccines to prevent and ultimately eliminate tuberculosis. Four vaccine candidates in Aeras' portfolio are currently in clinical trials in Africa, Europe and the United States, including two candidates in Phase IIb trials. Aeras receives funding from the Bill & Melinda Gates Foundation, the governments of the United Kingdom and the Netherlands, the Research Council of Norway, the State of Maryland, and other donors.

Jim Connolly joins Aeras after more than two decades of pharmaceutical industry experience. As Executive Vice President and General Manager of Wyeth Vaccines from 2004 to 2009, he played a leading role in expanding access to the breakthrough pneumococcal vaccine Prevnar to more than 100 countries and 35 national immunization programs, including numerous emerging and developing countries, where pneumococcal disease is a major cause of child mortality. He worked in cooperation with the GAVI Alliance and key stakeholders on the development and launch of the pilot Advance Market Commitment for pneumococcal vaccines. He was closely involved in the launch of Prevnar in Rwanda and The Gambia, the first developing countries to establish national immunization campaigns against pneumococcal disease. He also served on an advisory committee for the GAVI Alliance, a public-private partnership dedicated to improving world health by ensuring access to immunization in developing nations while supporting development of new vaccines.

Dr. Julian Lob-Levyt, the CEO of the GAVI Alliance, said, "I am delighted to learn that Jim Connolly has been appointed as President and CEO of the Aeras Global TB Vaccine Foundation. Aeras is fortunate to have him as its new leader. I am confident he will apply his effective and creative leadership to accelerate efforts to develop vaccines against TB, a devastating disease of poverty."

In the course of his career at Wyeth, Jim Connolly held a number of increasingly senior management, commercial and finance positions, including President and Managing Director of Wyeth Canada; Area Business Director for California and Nevada; Business Director of Wyeth's disease management joint venture with Merck-Medco; and Director of Finance for Wyeth Pharmaceuticals. He is a graduate of Washington University in St. Louis, Missouri, with a degree in Business Administration.

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Saturday, June 19, 2010

CNS coverage from "Research and development of new TB vaccines" Symposium, Zaragoza, Spain

Babs Verblackt wrote on issues around the tuberculosis (TB) vaccines, on-site from the "Research and development of new TB vaccines" Symposium, Zaragoza, Spain (3-4 June 2010). Babs is freelance journalist, a Fellow of CNS Writers' Bureau and Associate Communications at TuBerculosis Vaccine InitiativeTBVI). Read more



These CNS articles were published in a diverse range of media outlets of many countries including: India, Pakistan, Thailand, Sri Lanka, Nepal, Brunei Darussalam, Ghana, United Arab Emirates (UAE), USA, New Zealand, Bangladesh, South Korea, among others. CNS also used social media extensively to disseminate articles through Twitter (3000+), Facebook (2600+), younews, reddit, Google Buzz, Digg, newstrust, HealthDev.net, AIDSspace, nowpublic and others. These articles were also disseminated via electronic discussion forums on specific issues like SEA-AIDS, Stop-TB, Lung Health, to name a few. Synopsis of these articles was translated in Thai language and broadcasted through FM 102.5 in Thailand.

Three CNS articles written by Babs Verblackt, from the "Research and development of new TB vaccines" Symposium, Zaragoza, Spain, are as follows:

Thanks

Tuesday, June 8, 2010

Symposium shows progress in TB vaccines

Babs Verblackt writes for CNS from "Research and development of new TB vaccines" Symposium, Zaragoza, Spain
Steady progress is made in the development of new vaccines against tuberculosis (TB), researchers showed at a symposium in Spain. Several vaccine candidates are now being or soon will be tested in people.

European scientists gathered at the international symposium "Research and development of new tuberculosis vaccines" in Zaragoza, Spain, to share and discuss the progress in vaccines against the airborne infectious disease. At the second and last day (4 June 2010), Professor Stefan Kaufmann of the Max-Planck-Institute for Infection Biology in Berlin, Germany, illustrated that TB infection is a vicious circle: Each day about 125,000 infections result in roughly 25,000 TB cases, or 10 million new cases of TB disease a year. Around 5,000 people die of tuberculosis every day. Drug resistant TB strains, and HIV/TB co-infection further challenge global TB control. Read more



Kaufmann emphasized that vaccines can play an important role in turning the tide. He referred to studies showing that a 40-50 percent reduction in TB could be achieved by new vaccines. Improved drugs could lead to 10-27 percent reduction and better diagnostics to a 13-42 percent drop.

He elaborated on the development of the VPM1002 vaccine candidate by his team. VPM has successfully completed tests on safety and immunogenicity in Germany. Further trials (phase Ib) are taking place in South Africa at the moment.

Also in Spain progress is made. "It is a difficult process from research to development," Professor Carlos Martin of the University of Zaragoza said, describing the development of the MTBVAC01 vaccine candidate discovered by him and his colleagues. After more than 10 years of discovery and proof of concept and now 4 years of development, the vaccine is taking its first steps out of the lab: The vaccine is scheduled to be tested in people (phase I safety trials) the end of next year.

Dr.Jelle Thole, director of TuBerculosis Vaccine Initiative (TBVI), in a meeting with Spanish journalists called MTBVAC01 a leading vaccine in its kind. "It is the only candidate derived from the actual bug that starts tuberculosis. All other vaccine candidates either are based on improving or boosting BCG," he explained. TBVI, a European research consortium for the development of new TB vaccines, aims to have 8 vaccines in phase II safety and efficacy trials in 10 years.

New vaccines are aimed to improve or replace BCG, the only currently available vaccine against tuberculosis, which "does not protect against the most prevalent form of the disease, and therefore has little - if any - impact on the epidemiology of TB," Kaufmann said.

However, Martin stressed that BCG, developed in the 1920s, is "still in use because it is protective in children. In this regard, new vaccines should be at least as good as BCG in protecting against severe diseases as meningitis and miliar tuberculosis, and better in protecting against respiratory forms of the disease."

Worldwide new tools against tuberculosis are in several stages of development. Jan Gheuens, a senior program officer on the tuberculosis team at the Bill & Melinda Gates Foundation, summarized at the symposium: "Two vaccines are in large clinical trials, lots of vaccines are in other phases. Furthermore, 8 drugs are in pre-clinical development or further. And there is much excitement on the performance of a TB molecular diagnostic test."

Gheuens briefly mentioned strategic challenges to be considered. "What will be the next generation of new vaccines? New antigens or a new approach to vaccines? What about the cost of progress, can we raise the funds for larger clinical studies?" he questioned, adding that fundraising is 'tough' and that not just greater awareness of the challenges in TB, but also (public/political) commitment is needed.

The two day symposium (3-4 June 2010) was organized by the University of Zaragoza, the foundation Ramon Areces and TuBerculosis Vaccine Initiative (TBVI).

Babs Verblackt
(The author is a freelance journalist, a Fellow of CNS Writers' Bureau and Associate Communications at TuBerculosis Vaccine InitiativeTBVI)

Published in:
Thai-India News, Bangkok, Thailand
Asian Tribune, Sri Lanka
Elites TV News, USA
News Trust News, USA
Citizen News Service (CNS), India/Thailand
Arab News
Wikio.com, UK
Lankanewsheadlines.com, Sri Lanka
Bihar and Jharkhand News Service (BJNS)
Healthdev.net
Allvoices.com
CNS Stop TB Initiatives
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Thursday, June 3, 2010

Further research into field of new tuberculosis (TB) vaccines needed

Babs Verblackt writes for CNS from "Research and development of new TB vaccines" Symposium, Zaragoza, Spain
The development of new vaccines against tuberculosis (TB) is progressing in promising ways, but many issues remain to be further researched, European scientists explained on 3 June 2010 at a symposium in Spain.

At the first day of the International Symposium "Research and development of new tuberculosis vaccines" in Zaragoza, Spain, researchers reinforced the need for new vaccines against tuberculosis (TB), pointing out that TB is a continuously growing health problem and the only currently available vaccine, BCG, has limited efficacy in adults and safety issues in HIV-infected newborns. Read more


"I don't need to remind people here of the state of the problem," said Dr Ann Rawkins of the Centre for Emergency Preparedness and Response of the Health Protection Agency, United Kingdom, referring to the 2 million TB-deaths and 9 million new TB cases worldwide per year. "The international goal of elimination of the [TB] disease by 2050 can not be reached unless we get new diagnostic tests, new drugs and new vaccines. A large number of new vaccine candidates are currently at various stages of development."

The BCG vaccine is widely used and given to newborns worldwide. It protects against severe forms of childhood TB. But BCG has little to no efficacy in preventing pulmonary TB in adults, the most common and most infectious form of TB worldwide. Furthermore, because of safety issues in HIV-infected newborns, the World Health Organization (WHO) advises not to use BCG in babies known to be infected with HIV.

Research into new TB vaccines either aims to improve the BCG vaccine, to boost the immunity BCG gives, or to replace it. Professor of Immunology Hazel Dockrell of the London School of Hygiene and Tropical Medicine stressed the need to know exactly what the BCG vaccine is doing. "BCG has been around for a very long time, it was first given to a child in 1921, it is surprising we don't know more about it," she said, elaborating on various questions surrounding BCG. "We need to understand what sort of immunity BCG gives and what features of BCG should be improved."

Research done by Dockrell and colleagues shows that both young adults and infants in the United Kingdom and Malawi give a different sort of immune response to BCG vaccination. "That matters because many new vaccines now in development are boosting vaccines, aiming to improve BCG. But will they work better than BCG in areas where BCG itself doesn't induce good protection?"

Professor Paul-Henri Lambert from the University of Geneva stressed the importance of safety issues for new TB vaccines. "Rare adverse events can kill newly developed vaccines. A theoretical risk of safety issues has often hampered the development of a new vaccine. And unjustified allegations can lead to limiting use of a good vaccine," he said.

Prof Douglas Young, Fleming Professor of Medical Microbiology at the Imperial College in London highlighted the importance of more diversity in TB vaccine research. Most vaccines currently in development focus on boosting the body's natural immune response. "But it might as well be that the vaccines we're making at the moment are exactly the vaccines TB wants us to make," Young warned.

"TB might be perfectly happy with the way the natural immune response works, getting enough opportunities to transmit," he said, elaborating on the global diversity of TB strains and how these strains orchestrate the body's immune reaction. While current research is centered around cell-mediated immunity, "there is a landscape of diversity which is not yet exploited" Young said, encouraging his fellow scientist not to neglect the immense variety of immune response.

The symposium on new TB vaccines is being held during 3-4 June 2010 and is organized by the University of Zaragoza, Spain, the foundation Ramon Areces and TuBerculosis Vaccine Initiative (TBVI).

Babs Verblackt
(The author is a freelance journalist, a Fellow of CNS Writers' Bureau and Associate Communications at TuBerculosis Vaccine Initiative - TBVI)

Published in:
Modern Ghana, Accra, Ghana
Citizen News Service (CNS), India/Thailand
The Colombo Times, Colombo, Sri Lanka
The Asian Tribune, Sri Lanka
Elites TV News, USA
News Trust News, New Delhi, Delhi
Bihar and Jharkhand News Service (BJNS)
Banderas News, Mexico
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World Care Council
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Little About
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Wednesday, May 26, 2010

Omololu Falobi Award to Charles Shagi from Tanzania

To listen to the audio podcast of 2010 Omololu Falobi Award ceremony (at the M2010 closing ceremony) click here
"Omololu Falobi lived life only for 35 years. Yes he was in a hurry. He was a visionary. For those who knew him they would realize that this conference was part of his vision. M2010 is a turning point where it has become glaringly obvious that developing and rolling out new HIV prevention technologies is as much about community voices, politics, media, culture as it is about science. That's what Omololu thought of, that's what he dreamed of" said Manju Chatani Gada, at the closing ceremony of the International Microbicides Conference (M2010) in Pittsburgh, USA. Manju represents AVAC: Global Advocacy for HIV Prevention, African Microbicides Advocacy Coalition (AMAG) and has demonstrated a rich experience of community-centric responses to AIDS globally. Read more


"Omololu was killed in October 2006 in Lagos, Nigeria. He was a powerful international activist, a gifted journalist, a friend, a father, and a force to be reckoned with when it came to community activism. He founded and led the Journalists' Against AIDS in Nigeria (JAAIDS) and was instrumental in establishing several coalitions including the New HIV Vaccine and Microbicides Advocacy Society. His vision was of Africans to have a say in the issues that affected their lives and community advocates everywhere to be involved in shaping the response to AIDS" said Manju Chatani Gada.

"The field is growing fast and changing and many new faces are in this room. Perhaps many of you may not have been privileged to know Omololu. But rest assured, some project you know of, some network you are part of, some journalist who has covered your research, was touched by him. His vision lives in in the form of Omololu Falobi Award for Excellence in HIV Prevention Community Advocacy" said Manju Chatani.

The award was created to have an ongoing legacy to recognize the commitment of HIV prevention research advocates. The award was established by the African Microbicides Advocacy Group (AMAG), in partnership with AVAC, the Global Campaign for Microbicides (GCM), Journalists Against AIDS (JAAIDS) and the New HIV Vaccine and Microbicides Advocacy Society. We thank a number of supporters including AMAG, AVAC, Family Health International (FHI), Global Campaign for Microbicides (GCM), NHVMAS and the joint United Nations programme on HIV/AIDS (UNAIDS)

While sharing her memories of how the screening committee selected the 2010 Omololu Falobi Award for HIV Prevention Community Advocacy, Manju Chatani Gada said: "One member of the screening committee said 'it was an easy choice. He is an epitome of science meets advocacy'. The 2010 Omololu Falobi Award for HIV Prevention Community Advocacy goes to Charles Shagi from Tanzania."

"Omololu was an incredible man" said the inaugural recepient of 2008 Omololu Falobi Award for HIV Prevention Community Advocacy Lori Heise. "Charles' enthusiasm is infectious and he has been committed to helping recruit and mentor new people to the movement to expand the range of HIV prevention options," said Lori Heise, former Executive Director of the Global Campaign for Microbicides and one of the inaugural recipients of the award and member of the 2010 selection committee. "We need more people like Charles who can ably bridge the gap between researchers and community members."

I couldn't have agreed more for having had the privilege to work closely with Omololu in early 2000s on HIV prevention advocacy. Lori was indeed a symbolic choice for thousands of people at least who are committed to push HIV prevention advocacy on daily basis.

The 2010 recepient of Omololu Falobi Award for HIV Prevention Community Advocacy, Charles Shagi, is a community educator who developed innovative ways to link women in Tanzanian villages with life-saving HIV prevention information and with HIV prevention research trials. Charles Shagi, a Program Officer for the African Medical and Research Foundation based in Mwanza, Tanzania, was honored for his significant contributions to developing and sustaining community engagement and education programs that empower women and their communities to advocate from themselves and to become vital partners in HIV prevention research trials.

"Bringing HIV prevention research to communities is an essential part of our work to develop new HIV prevention options for men and women," said Sharon Hillier, Microbicides 2010 Co-chair and a member of the award selection committee. "Charles embodies what this award was created to recognize: leadership, commitment and passion in community advocacy. He works tirelessly not only to help women advocate on their own behalf and to become involved in research, but also to educate and empower researchers to understand the needs of women, their families and communities."

Charles works tirelessly not only to help women, their families and their communities advocate on their own behalf and to become involved in research.

"I am very humbled to accept this award, and for me, it really underscores the value this field put on the importance of reaching out to the women. – in the villages of Tanzania and around the world – who participate in these trials" said Shagi. "This award is important because it proves that people do care about them. It is the courage of those women that is being honored today. I look forward to continuing to share the voices and experiences of vulnerable women with the research and advocacy communities."

"I urge all HIV prevention researchers to listen to the community. There is need for all of us to change attitude, but especially the researchers and our leaders since we have a long walk left. Communities should be at the center of research, not at the periphery," Shagi added.

The Omololu Falobi Award highlights the essential role of community advocacy and leadership in HIV prevention research. It celebrates the life and values of the late Omololu Falobi, a long-time HIV advocate and journalist who founded Journalists Against AIDS in Nigeria, was an instrumental pioneer member of the Nigerian Treatment Access Movement, and co-founded the New HIV Vaccine & Microbicide Advocacy Society. Omololu was killed in Lagos, Nigeria in October 2006. The award was conceived as an ongoing legacy that recognizes his commitment and lasting contributions to HIV prevention research advocacy.

"Omololu was a visionary leader and activist, who accomplished much in his too short a life.  He dedicated himself to powerful advocacy for HIV and HIV prevention research in Nigeria, Africa and worldwide," said Funmi Doherty of NHVMAS in Nigeria. "It is gratifying to see his ideals and vision live on through this award. I know he would be immensely proud of the work that Charles and the past recipients are doing to simultaneously advance human rights and HIV prevention research."

Shagi was chosen from among an impressive group of almost 20 nominees by an independent international panel of HIV prevention research advocates, policy makers, and scientists. The selection committee noted his instrumental role in pioneering new ways to bring the voices of community members and participants into the research process.

Charles and his colleagues have also documented and published peer reviewed articles about their model for community representation and participation in HIV prevention trials among women.  This research is an important guide for those working on community engagement plans for HIV prevention trials around the world.

Bobby Ramakant - CNS

Sunday, May 23, 2010

State of the ART of microbicides

To listen to the audio podcast of Prof Robin Shattock click here
The microbicides field has undoubtedly moved and shifted a lot in the past decade. Now, with first generation microbicides candidate products up and gone, antiretroviral treatment (ART)-drug based microbicides in spotlight, and only three major microbicides efficacy studies remaining, the need to lobby for increased funding of microbicides research and development, was never so compelling.

The need to bolster HIV prevention has certainly not dimmed - and so has the need to up HIV treatment, care and support which is becoming acute on daily basis. The International Microbicides Conference (M2010) opened with the plenary that cited UNAIDS data, from New York Times news (At Front Lines, AIDS War Is Falling Apart), "For every 100 people put on antiretroviral treatment (ART), 250 people are getting newly infected with HIV." Read more


"People were already questioning that whether universal access to treatment is achievable without significantly reducing the number of new infections" said Professor (Dr) Robin Shattock, who is a Professor of Cellular and Molecular Infection in the Department of Cellular and Molecular Medicine at St George's University of London, UK.

"Donors were questioning too whether it is sustainable to continue the roll out of treatment across the globe" said Prof Shattock.

There is no doubt that HIV prevention, treatment, care and support programmes all need to be fully funded, supported, and rolled out in all possible ways so as to reach the hardest-to-reach affected communities.

FIRST MICROBICIDES CONFERENCE TO TALK ABOUT HIV PREVENTION TECHNOLOGIES IN A BROADER CONTEXT
"This is the first microbicides conference to talk about HIV prevention technologies in a broader context. It also includes Pre-Exposure Prophylaxis (PrEP) and really the two fields of microbicides and PrEP are starting to become very blurred" said Prof Shattock.

"The research is going on taking the same tenofovir based drug orally to prevent infection or applying a similar drug topically - the distinction between PrEP and microbicides have become more blurred" said Prof Shattock.

THAI AIDS VACCINE TRIAL MUST BE REPLICATED
In September 2009, the world's largest AIDS vaccine trial (Thai Prime-Boost study) to date showed the first evidence that an experimental AIDS vaccine could lower the risk of HIV infection. The results were complex; the observed benefit from the vaccine was modest; and the field is still years away from a highly protective vaccine. "The caveats to the Thai Prime-Boost study results are important and true. But letting them become the entire story does a severe, even dangerous, disservice to the field, the trial and especially the 16,000 people who participated in the trial," said Mitchell Warren, Executive Director of AVAC: Global Advocacy for HIV Prevention.

"The Thai AIDS Vaccine trial needs to be repeated which could change things dramatically" said Prof Shattock.

MOVES AND SHIFTS IN MICROBICIDES FIELD
"With microbicides, when the first generation microbicides were successfully tested, and we should not underestimate what a significant advancement it was, but it appears to either lack sufficient potency or not be used appropriately enough to show statistical end-points" shares Prof Shattock.

"Then it led the microbicides field to move towards potent products specifically those that are targeted against the virus. It also shifted the microbicides field to develop a programme of systematically testing the biological plausibility of different targets in the primate model to validate whether a target is appropriate for prevention approaches. It also accelerates and emphasizes the need for drug distribution studies and tissue activity studies in both primates and humans. It also led the microbicides field to prioritise new formulations that maximise adherence to give the best possible chance of showing efficacy in a clinical trial" explains Prof Shattock.

"These developments led to increasing emphasis on combination products. Combination products not only to ensure that any microbicide will hit the wide possible diversity of virus but also potentially to reduce the risk of resistance" said Prof Shattock.

"It has also led us to recognizing the need to prioritise several efficacy testing in clinical trials because it is only human data that already helped us understand when the basic science is pointing us in the right direction" added Prof Shattock.

CRITICAL STANDPOINT IN MICROBICIDES DEVELOPMENT
"So right now at this conference I believe we stand at the critical standpoint in microbicides development, critical because the first generation products have been and gone, and next generation products are poised to be tested in clinical trials, that represents quite a vulnerable position to the field because without some proof of efficacy in future trials it may become harder and harder to sustain funding for microbicides development" said Prof Shattock.

With ART based microbicides, there is a need to have appropriate drug delivery mechanisms - Many of these ART targeted microbicides are operating at the level of preventing HIV infection at the target cell, which means it needs to be delivered at the right time at the right tissue. But also can be taken for combination with products that have a high barrier for resistance and will have a limited impact on therapy.

"What we do know is that the transmission takes place very rapidly. So it is absolutely critical for the science of microbicides development, to make sure the product is there, covering and protecting the target cells, at the time of exposure" said Prof Shattock.

There are many antiretroviral drugs already being used in HIV treatment and this is perhaps the biggest success story in HIV history with development of as many ART drugs as the number of years have passed by since the discovery of HIV. "This also means significant investment into research and drug development that has gone over years.

"One reason for engaging antiretroviral drugs into microbicides development is to accelerate the candidates that are ready to go into clinical trials because they come from a very rich product development profile. So now we have so many good candidates, can we provide the much needed bridge to establish biological plausibility - to find out will these things actually work in clinical trials" said Prof Shattock.

"So we now have extremely good biological plausibility that microbicides could work and how can we use this knowledge in performing better human trials. Well more emphasis is being placed on drug distribution and tissue activity studies and we hear people talking about PK and PD. Pharmacokinetics (PK) is how much drug is needed and where is it needed to provide protection. Work is also being done to determine tissue drug activity - Pharmacodynamics (PD) - whether the drug which is delivered is active" explains Prof Shattock.

BEST CHANCE OF SEEING EFFICACY IN A CLINICAL TRIAL
Prioritisation of new products is receiving particularly more attention in order to maximise adherence so that we have the best chance of seeing efficacy in a clinical trial. And this has led many people to trying to move microbicides from time-of-exposure products to pre-exposure products.

ARV-based Microbicices be prescription-only products?
Should ARV based microbicides be prescription only product? This sounds disappointing especially for those who came from microbicides field because the original vision was to have an over-the-counter (OTC) product. But the benefit of prescription-only product that requires testing is that it will have a positive impact on the voluntary counselling and testing.

Emphasis will be placed on a combination that reduces the threat of resistance. "It is not entirely inconceivable that if we have an ART-based mono-drug product that shows efficacy that eventually it could become an over-the-counter (OTC) product" said Prof Shattock.

LACK OF SUFFICIENT FUNDING IN MICROBICIDES FIELD
We are at the advent of multiple different products, multiple different delivery strategies, but lack of sufficient funding to take them all to the clinical trials. So we need to be very smart on what goes into the efficacy trials. This has led the field to prioritising on what's best-in-class. So how do we go about choosing the best in class?

Firstly we need to choose the best-in-class inhibitor in a different category. There is no sense of testing multiple drugs in the same category.

Secondly, we need to choose at the level of potency and selectivity.

Thirdly, these products need to be stable.

Fourthly, looking at products that reduce resistance and can combine with other drugs, will be prudent.

Fifthly, we need to look at the stage of development of this product - if we don't have a product that shows a degree of efficacy in the next five years, some product 10 years behind the queue will never have the opportunity to try a clinical trial.

And many such factors that scientists use to prioritise different potential microbicides candidate products.

"There are only three potential microbicide efficacy trials remaining... now that is quite concerning because although there is a strong biological plausibility we all know that science is full of surprises. And efficacy is not just about potency of the drug, but also about the way it is delivered and the way it is used" said Prof Shattock.

"Many of you are aware that after the Thai AIDS Vaccine trial, the vaccine advocates are lobbying to get funding to do a phase 2b trial every year, whether they will be able to get the money for that is debatable but I don't see microbicides field standing up and lobbying hard enough to do more clinical trials to get the human data that will inform the basic science" said Prof Shattock.

Some new data on ART-based microbicide studies may be announced at the forthcoming International AIDS Conference, Vienna, Austria. 2009 Thailand's AIDS Vaccine study results were promising indeed. Yet there is a very long way to go for the HIV prevention research field and perhaps, might succeed in turning the tide of the new HIV infection.


Bobby Ramakant - CNS


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