Press Release

AVAC Applauds Biden Administration Repeal of the Global Gag Rule

AVAC calls for further reforms to support women’s health programs and the fundamental human right of reproductive choice and health access

Contact

Kay Marshall, +1 (347) 249-6375, kay@avac.org

New York City, January 28, 2021 — AVAC applauds the executive action taken today by US President Joe Biden to repeal the Mexico City Policy, also known as the Global Gag Rule (GGR), which prohibits many foreign groups receiving US foreign aid from speaking about, referring for, advocating for access to, or providing abortion. The GGR has had an enormous deleterious effect on US-funded global health work and led to loss of life and harm to cisgender women, adolescent girls and young women worldwide.

As COVID-19 exacerbates gender-based violence, disrupts contraceptive programming and threatens HIV prevention for women in all their diversities, this repeal is a welcome, necessary action—and must be the first step in broad, bold US government commitment to the health and wellbeing of girls and women.

There is much more that needs to be done now to undo the damage done by the policy, including immediate communication about the repeal, and proactive outreach to ensure partners who declined US funding while the GGR was in place are brought back into US-supported networks of prevention, care and support. Steps must also be taken to ensure that the GGR is eliminated as an option for controlling women’s health programming. AVAC stands in solidarity with allies, including Health GAP, who have been clear in demanding that the Biden Administration correct the extensive harms already done and end this cycle by establishing a permanent policy that supports sexual and reproductive health and rights for all, in the US and globally.

Four years ago, the Trump Administration reinstated and expanded the GGR (originally enacted by Ronald Reagan in the 1980s and reinstated in all successive Republican administrations). The Trump expansion of the Global Gag Rule vastly increased the range of groups subjected to its lethal restrictions. As it has in every prior era, the 2016-2020 imposition of the GGR resulted in increased unintended and high-risk pregnancies, unsafe abortions and maternal deaths, and hampered introduction HIV and sexual and reproductive health and rights programs that are urgently needed worldwide. It will take years to rebuild the programs that were damaged by this policy, and the damage done to women’s lives is incalculable.

The Biden Administration must ensure immediate, multi-channel communication with partners about the repeal of the GGR; it must also launch an urgent review of all federal guidance and rules to purge the references to the GGR that may still affect funding and programs. The Office of the Global AIDS Coordinator must immediately clarify that section 5.9.4 of its 2021 Country Operational Plan guidance on implementation no longer applies, including to plans for the coming year. The administration must also allow PEPFAR funds to be used to procure a range of contraceptives beyond condoms, as is the current policy. Women’s health should not be divided between one clinic to access HIV treatment or prevention and a separate one to access contraceptives and other sexual health interventions. It is past time for PEPFAR to support integrated health options for women, especially in the context of the COVID-19 pandemic.

Along with expanding PEPFAR support, the administration should immediately reinstate funding for UNFPA to help ensure increased and sustained funding for contraceptive options for women.

The Administration must also work with the US Congress to ensure that the GGR is permanently legislatively repealed so that it cannot be easily reinstated by a future administration. To this end, the Administration should enthusiastically support the Global Health, Empowerment and Rights (HER) Act, which was introduced today by bi-partisan leadership in the House and Senate and would ensure the US could make permanent and long-lasting partnerships in support of women’s health and rights without fear of programs being rolled back with each new administration.

The Biden Administration has spoken of a desire to dismantle white supremacy and racist structures in the US. That commitment must extend to its foreign policy and development programs. For too long, US global health and development support has relied on policies and programs that at their worst are colonialist and antifeminist. Repealing the GGR is an important step in the right direction, but AVAC looks to the Biden administration to work with advocates and public health experts to examine all current policies and programs with a lens of anticolonialism and human rights and make the necessary changes to truly bring US foreign policy for health and development into the 21st century.

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About AVAC: Founded in 1995, AVAC is a non-profit organization that uses education, policy analysis, advocacy and a network of global collaborations to accelerate the ethical development and global delivery of HIV prevention options as part of a comprehensive response to the pandemic. Follow AVAC on Twitter @HIVpxresearch.

Press Release

Data from Antibody-Mediated Prevention Studies Advance the Field and Show the Challenges that Lie Ahead

HIV Research for Prevention Conference Presents Important Research Insights Across a Range of New Options

Contact

Kay Marshall, +1 (347) 249-6375, kay@avac.org

New York City, January 26, 2021 — Today at a press conference hosted by the HIV Research for Prevention (HIV R4P) conference, research teams presented a range of data from ongoing studies of antibody-mediated prevention, long-acting injectable PrEP, a monthly PrEP pill, and trends in daily oral PrEP use. Together, they point to a future of biomedical HIV prevention research and programs with a greater understanding of mechanisms of prevention, enhanced trial designs and a wider range of prevention options.

HIV R4P Virtual 2021 begins officially on January 27th. Today’s press conference offered top-line findings from the full scientific presentations that will be made later this week. These data have not yet been published in peer-reviewed journals but warrant close attention for their implications for the field.

At the press conference, researchers from the NIH-funded HIV Vaccine Trials Network (HVTN) and HIV Prevention Trials Network (HPTN) presented initial data from the Antibody-Mediated Prevention (AMP) trials of an HIV-specific broadly neutralizing antibody (bNAb) called VRC01, delivered intravenously once every eight weeks. The trials enrolled cisgender women in sub-Saharan Africa and gay men and transgender persons who have sex with men in Brazil, Peru, Switzerland and the United States. According to Larry Corey, AMP Studies protocol chair and principal investigator of the HVTN, VRC01 did not significantly reduce the overall risk of HIV acquisition in participants who received the antibody compared to those who received the placebo. However, VRC01 did safely and effectively reduce the risk of acquiring HIV strains classified as “highly-sensitive” to neutralization by VRC01.

“These were complex and well-designed trials of a novel HIV prevention concept, and the results move the field forward in important ways,” said Mitchell Warren, AVAC Executive Director. “The AMP trials show that a broadly neutralizing antibody can reduce the risk of acquiring viruses that are very sensitive to that antibody. This is welcome news; it is the first evidence in humans that intravenous infusions of a broadly neutralizing HIV antibody can reduce a person’s risk of acquiring HIV via sex.”

The AMP results also demonstrate the extent of the challenge that lies ahead for antibody-mediated prevention. There are multiple strains of HIV circulating through communities. The trial team used lab tests to predict how many HIV strains in trial communities would be sensitive to, and blocked by, VRC01. The trial data didn’t match these predictions. Fewer viruses were highly-sensitive to VRC01 than the AMP team had hoped. The trials showed that a bNAb like VRC01 does not offer sufficient protection on its own and that a combination of bNAbs is likely needed if broad protection is to be achieved.

“AVAC is grateful to the research teams, trial participants, clinic staff and community advocates who made these trials possible. The next step for the prevention field is to determine how these results can be used to guide the selection of combination bNAb products to advance to efficacy trials. Advocates should monitor — and be engaged in — these deliberations,” said Stacey Hannah, AVAC’s Director of Research Engagement.

“With new prevention options like the Dapivirine Vaginal Ring and injectable cabotegravir for PrEP advancing towards licensure, people at risk of HIV will have more choices. This is a great thing. As choice expands, efficacy trials of future products will need to be designed in new ways, and advocates’ support for investigation of bNAbs as part of this prevention pipeline is crucial,” said Hannah, who also led the development of AVAC’s Advocates’ Trial Design Academy that is engaging with developers and trial designers in considering the future.

Participants in the AMP trials received one of two different doses of VRC01 or a placebo administered every eight weeks via intravenous infusion. Some participants — in both the placebo and VRC01 arms — acquired HIV in spite of counseling, condom provision and PrEP referrals and counseling at all study sites. Viruses from these participants were isolated from their blood samples, sequenced and analyzed in the laboratory to determine the concentration of VRC01 that blocked viral activity. Viruses neutralized with a <1 microgram/mL, a measure of the virus’s susceptibility to neutralization by VRC01, were classified as highly-sensitive. Participants who received VRC01 were significantly less likely to acquire a virus highly-sensitive to VRC01 compared to those who received the placebo. For viruses with a sensitivity greater than 1, no statistically significant protection was observed.

Importantly, the study’s findings have shown that a specific test, or assay, used in the study may predict whether future antibodies are likely to provide protection against a broader range of HIV sensitivities when used alone or in combination. The identification of such an assay that can be used to evaluate whether the future bNABs, alone or in combination, are likely to protect is an important step forward for the field and may help predict the combination and amount of antibodies needed for protection.

In the press conference update, AMP investigators reported that no difference in trial findings across gender and in the context of regions where clade B and clade C predominate (HVTN 704 and 703 trials, respectively.) This is the first time that a trial in humans has shown that an intravenously-administered bNAb reaches the mucosal surfaces where sexual exposure occurs, and that it can protect at these surfaces.

The AMP results were presented alongside other important HIV prevention advances, including interim results of the HPTN 084 efficacy study showing safety and efficacy of injectable cabotegravir amongst cisgender women presented by Sinead Delany-Moretlwe, protocol chair, director of research at Wits Reproductive Health and HIV Institute. The data also provided more information on how injectable CAB-LA compared to daily oral PrEP in terms of reducing risk of HIV. The investigators reported that, while rates of HIV in cisgender women were low in both trial groups, CAB-LA was more effective than daily oral PrEP. The efficacy a product shows in a clinical trial is just one factor affecting its effectiveness. As the contraceptive field has long known, the most effective product is the one that fits into a person’s life and is used. HPTN 084 provides more information to help cisgender women make informed choices.

At the press conference, Sharon Hillier of the Magee-Women’s Research Institute at the University of Pittsburgh reported on an interim analysis of the Phase 2a trial of the once-monthly pill form of the antiretroviral Islatravir, which found it to be safe and well-tolerated, with presence in the blood over time that researchers believe will correlate with protection. Islatravir is moving into efficacy trials in 2021.

An analysis of oral PrEP uptake data from AVAC’s Global PrEP Tracker, showed increased initiation of daily oral PrEP, even in the midst of the COVID-19 pandemic, but also noted that the rate of increase is slowing down — a sign that work must be done to ensure expanded uptake of existing options even as new ones become available Kate Segal, Program Manager for Product Introduction and Access at AVAC said, “Many of the countries with the highest PrEP initiations exhibit shared traits that have contributed to their success with scaling up PrEP: early adoption of PrEP, national commitment to scale-up, and programs tailored to populations at high risk offering community-led, accessible, non-discriminatory services and linkages to social support.”

“Taken together, this suite of studies being presented at HIV R4P offer a set of clear imperatives for HIV prevention: national governments, funders and advocates must work to continue to increase access to daily oral PrEP; and work to ensure that today’s PrEP programs provide a platform for tomorrow’s products, including injectable cabotegravir and the Dapivirine Vaginal Ring. At the same time, research must continue, including efficacy trials of Islatravir and other next-generation PrEP options and research that builds on the AMP results to inform both antibody and vaccine development,” Hannah said.

AVAC looks forward to working with researchers, funders, policy makers, advocates and activists to ensure that the results of these trials are translated into impact.

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Press Release

US FDA COVID vaccine authorization important step toward ending the COVID-19 pandemic

AVAC and TAG call for global cooperation to ensure equitable rollout of vaccines and other COVID-19 interventions

Contact

Richard Jefferys: richard.jefferys@treatmentactiongroup.org
Kay Marshall, +1 (347) 249-6375, kay@avac.org

New York City, 11 December 2020 – Today’s decision by the US Food and Drug Administration (FDA) to grant an Emergency Use Authorization (EUA) for the Pfizer-BioNTech mRNA vaccine is an important step toward bringing the COVID-19 pandemic under control in the United States. The US joins Bahrain, Canada, Mexico, Saudi Arabia and the UK in granting regulatory authorization of the Pfizer-BioNTech vaccine. More countries are expected to authorize this vaccine in the coming days, and the FDA will next week consider an EUA for the Moderna mRNA vaccine. One or more other vaccines are expected to follow in the coming weeks and months, with potential for full regulatory approval for one or more by mid-2021.

An EUA is an important step in the race to get vaccines to all who need them. However, public health history shows that only fully and fairly deployed vaccines will actually end this pandemic. It is past time for a comprehensive global plan that provides a clear framework, funding and clear accountability for equitable access to everyone in the world, regardless of income and ability to pay.

AVAC and TAG call for action in three areas:

A robust, integrated research plan: Policy makers and public health programs need to start planning now for follow-on research related to follow-up of trial participants, expanded populations, operational research to optimize deployment, and the prevention of infection and onward transmission (in addition to prevention of disease). Regulators and trial sponsors must provide a plan for ethically continuing follow-up of participants in the Pfizer-BioNTech trials, including plans for when and how participants will be unblinded and placebo recipients will be offered the vaccine. National regulatory agencies, the World Health Organization, researchers, ethicists, and community representatives must develop recommendations for control arms of ongoing and planned COVID vaccine and prevention trials. In addition, vaccine developers, in conjunction with the FDA and other regulators and in consultation with communities, must articulate and implement a plan for accelerated vaccine research and regulatory review for populations not included in the original studies, including pregnant women and other people who are pregnant and children of all ages. We note that while the efficacy trial included a small number of people with HIV, safety data have yet to be reported due to insufficient follow up–these data should be made available as soon as possible, given that there are likely to be people living with HIV among the priority populations for vaccination.

Rational, fully-funded deployment plans in the US: Under the current administration, there is no well-articulated national deployment plan, and state and local efforts are starved of funding. The Trump administration must immediately begin to work closely with the incoming Biden administration to ensure a coordinated national plan that supports and fully funds local efforts. This must include community-led and -developed plans to build trust in vaccination programs, particularly among historically marginalized populations who have reason to distrust government-sponsored public health plans. These plans should include data-driven programming to ensure that populations most at risk of COVID and on the front lines of essential work have access to vaccines as quickly as possible. And these programs must have effective communication campaigns to address side-effects, safety, and potential adverse events to ensure that concerns, which will inevitably arise, are addressed in a clear, transparent, evidence-based and coordinated manner. Distribution plans must also include equitable vaccine allocation based on risk and need. In addition to the importance of vaccinating people whose age, profession, or preexisting conditions place them at high risk, incarcerated and detained populations have notably not been prioritized in COVID-19 vaccine distribution frameworks, and are absent from some preliminary State plans, despite being one of the most at-risk groups. Black, Latinx, indigenous, and other communities of color face high risk of COVID-19 and of poor outcomes from it due to entrenched structural and racial injustices, and also must be prioritized equitably.

Global commitments to equitable global access: COVID anywhere is COVID everywhere. Vaccine nationalism is unethical and is counterproductive to ending this pandemic. New data released this week shows that 9 out of 10 people in poor countries will not have access to COVID-19 vaccines in the next year, while the world’s richest countries have reserved up to 5 times as many vaccine doses as they need for their citizens. The US and other wealthy countries must abandon this vaccine nationalism and work with COVAX and other international programs to ensure equitable global access. In addition, the research pipeline must be optimized to speed development of vaccine formulations that will be easier to store and deliver in areas with underdeveloped health infrastructure. Vaccine manufacturing capacity must be enhanced, including technology transfer and waiving intellectual property protection during the pandemic, to ensure the maximum number of doses of safe and effective vaccines and in keeping with the massive public investments that have underwritten the development and distribution of these innovations.

In testimony at the FDA Advisory Committee hearing on Thursday, Mitchell Warren, AVAC executive director said: “The FDA process is not just about authorization or approval; it is a beacon of independent review and transparency that will help foster the trust necessary to re-build confidence in vaccines, in science and in our public institutions.”

“This is a tremendous step forward,” Warren said. “But if we’ve learned anything in almost four decades of fighting HIV, it’s that proven and approved interventions only reach those who need them most when there are well designed, fully funded programs to deliver them.”Mark Harrington, executive director of the Treatment Action Group (TAG), adds “the rapid development of safe, effective vaccines for preventing COVID-19 is a testament to what can be achieved with sound science, political will, and adequate resources. In addition to ensuring that all have access to these innovations in keeping with the human right to science, our governments must expand investments in research and delivery to ensure similar achievements to end other infectious pandemics, including HIV, tuberculosis, and hepatitis C.”

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About TAG: Treatment Action Group (TAG) is an independent, activist and community-based research and policy think tank fighting for better treatment, prevention, a vaccine, and a cure for HIV, tuberculosis, and hepatitis C virus. TAG works to ensure that all people with HIV, TB, and HCV receive lifesaving treatment, care, and information. We are science-based treatment activists working to expand and accelerate vital research and effective community engagement with research and policy institutions.

Press Release

Efficacy News from Second COVID-19 Vaccine Trial Underscores Need for Transparency and Cooperation between Outgoing and Incoming US Administrations

Americans are dying. Politics cannot be allowed to slow vaccine roll out.

New York City, November 16, 2020 — AVAC and Treatment Action Group (TAG) welcome today’s announcement that preliminary data from the efficacy trial of Moderna’s mRNA COVID-19 vaccine indicate a high-level of protection against COVID-19. This is much needed good news as the US and other countries continue to see dangerously rising rates of COVID-19. As our organizations expressed in a statement last week about the Pfizer mRNA vaccine news, caution is warranted in interpreting this preliminary information as we wait for additional data from Moderna and further actions from the US Food and Drug Administration (FDA) and other global regulatory authorities.

In light of these hopeful announcements, planning for distribution of both of these vaccines must be accelerated. In the US, that planning – and potentially the beginning of distribution – will span two presidential administrations. It is clear that on January 20, 2021, there will be a change in executive leadership, even while the election results have not been certified and the Trump campaign continues to baselessly contest the results through lawsuits in a number of states.

AVAC and TAG call on the Trump campaign and administration, senior elected officials in the Republican Party and the leadership of the Republican National Committee to put the lives of the American people ahead of politics and move to ensure that there is a smooth transition of power that focuses on transparency. The GOP must work hand in hand with the incoming Biden Administration to maximize the impact of the limited number of vaccine doses that are expected to be available late in 2020 and early 2021.

The Biden transition team has laid out plans for a comprehensive COVID response that give us hope that – especially with the deployment of highly effective vaccines where they are needed most – the pandemic may begin to be controlled in 2021. That work will be more effective and will save more American lives if the incoming administration has all possible information about stockpiles, distribution plans and other logistics along with the ability to meet with and work with current administration officials and state and local officials.

But there is also urgent work to be done by the current Congress and Administration. Deploying these vaccines will be one of the most ambitious public health undertakings in history. A comprehensive, fully-funded and nationally-directed deployment plan must be developed now to complement the billions of dollars invested and the time, talent and commitment of thousands of researchers and trial participants who gave us these results. Vaccine costs should reflect the significant contributions of public financing to their design and development. Congress must come together in a bipartisan way to ensure that the CDC and state and local health departments have the funding, technology, training and support needed to ensure that vaccines can be deployed as quickly as possible to reach the most at-risk populations, accompanied by appropriate, evidence-based and trusted public health information.

We have lost almost 250,000 Americans to this virus, and new infections are rising every day. It is past time to put American lives ahead of politics.

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Press Release

Landmark Trial in East and Southern Africa Finds Injectable PrEP Safe and Effective for Cisgender Women

Regulatory review and introduction plans must be accelerated

Contact

Kay Marshall, +1 (347) 249-6375, kay@avac.org

New York City, November 9, 2020 — AVAC enthusiastically welcomes the news that another trial of the long-acting, injectable antiretroviral cabotegravir (CAB-LA) for HIV prevention for HIV pre-exposure prophylaxis (PrEP) has demonstrated safety and efficacy, this time among cisgender women. Today’s announcement from ViiV, the US National Institute of Allergy and Infectious Diseases (NIAID), and the HIV Prevention Trials Network (HPTN) is based on a scheduled review by an independent data and safety monitoring board (DSMB) of the HPTN 084 study. Data reviewed by the DSMB found that CAB-LA provided significant protection from HIV. The trial also re-confirmed the safety and efficacy of daily oral TDF/FTC (brand name Truvada). Earlier this year, HPTN 083, a companion trial of CAB-LA among cisgender men and transgender women who have sex with men, reported similar results.

“This is extremely encouraging and exciting news for women around the world,” said Maureen Luba Milambe, AVAC’s African Regional Advocacy Advisor. “We congratulate the trial team and thank especially the more than 3,200 women from Botswana, Eswatini, Kenya, Malawi, South Africa, Uganda and Zimbabwe, whose participation in the study provided this important advance for HIV prevention.”

Data from the trial showed a clear protective benefit from cabotegravir, with an 89% percent risk reduction compared to oral TDF/FTC for PrEP. Overall incidence in the study was 1%, with 1.79% percent in the daily oral PrEP arm and 0.21% in the CAB-LA arm. Of 38 total HIV infections in the study, only four occurred among women who were receiving cabotegravir. Importantly, even though the rate of HIV infection was higher among women taking daily oral PrEP, 1.79% was the lowest incidence among women in a randomized trial of daily oral PrEP to date, underscoring the effectiveness of daily oral PrEP. Over the past 15 years, rates of HIV infection in HIV prevention trials in the region have consistently been closer to 4% when no active drug was provided. HPTN 084 demonstrates that both oral and injectable PrEP are safe and effective options.

As reported today, the HPTN 084 DSMB recommended that the blinded, randomized portion of the study be stopped early and all trial participants be told which active drug (CAB-LA or oral TDF/FTC) they were receiving as part of the study. The study will continue to completion with all participants being offered their preferred product.

“We now know that CAB-LA is highly protective against HIV for both men and women. The urgent work now is for policy makers, funders, program implementers and communities to design and build HIV prevention programs and health systems that can deliver the growing array of biomedical PrEP options, including oral, vaginal ring and injectable, and make them feasible choices for all people at risk of infection,” said Mitchell Warren, AVAC Executive Director. “This is essential work that can and must begin now, while we await further data, regulatory review and potential normative guidelines. Key to those efforts will be ensuring that we don’t repeat the delays that have slowed daily oral PrEP rollout over the past eight years.”

In preparation for the HPTN 084 study results, AVAC, along with a cadre of cisgender women in Africa, Europe and the US, have been working to identify potential issues, opportunities, challenges and concerns about the introduction of a new injectable HIV prevention product. This group will work with other networks of advocates for sexual and reproductive health and rights to continue to articulate an agenda for introduction of CAB-LA in the context of these welcome positive results.

“A new HIV prevention option for women is cause for celebration,” said Chilufya Kasanda Hampongo, a Zambian women’s health advocate with the Treatment Advocacy and Literacy Campaign (TALC). “We know that real choice depends on giving women—and all people—full information about risks and benefits, pros and cons of different methods, and of making sure that those methods are available for people to select from. An injectable will be a great choice for some people; for others, daily oral PrEP or the Dapivirine Vaginal Ring will be the right strategy for reducing HIV risk.”

“We must advance biomedical strategies in the context of comprehensive, community-led programs to deal with violence, stigma and discrimination. COVID-19 has shone a light on the epidemics of sexual and gender-based violence that help drive HIV,” said Yvette Raphael, Executive Director of Advocacy for Prevention of HIV and AIDS (APHA) in South Africa. “To be truly effective, injectable HIV prevention and other biomedical options must also be accompanied by investments in women-led work to break the cycles of violence in our societies.”

Advocates also emphasize the remaining need for significant work to understand how this new product can be effectively delivered in communities and among populations where it is most needed. Understanding user preferences, health system capacity needs, the price of the product and the programs that will deliver it, the potential risk of drug resistance and other issues are all critical parts of the puzzle that must be addressed as quickly as possible.

“In 2018, AVAC and the Clinton Health Access Initiative (CHAI) established the Biomedical Prevention Implementation Collaborative (BioPIC) to work with a wide range of stakeholders to develop an introduction plan for CAB-LA and other next-generation HIV prevention options. Today’s announcement gives new urgency to that work of translating promising research results into public health impact,” said Jessica Rodrigues, AVAC’s Director of Product Introduction and Access. “Operational research to find out how communities and individuals can best be supported to access the drug, and how health systems can be strengthened to deliver it should it be approved for use, is a critical next step and planning must begin now,” said Rodrigues.

Additional HPTN research is ongoing and is needed to understand safety and efficacy of CAB-LA for prevention among adolescent girls and pregnant and breastfeeding women, populations that are often at increased risk for HIV infection. In addition, while oral PrEP, the vaginal ring, and now injectable PrEP expand potential options, continued research is still needed on additional methods to expand options that can meet the needs of all populations.

“People need choices for HIV prevention that will work in their lives,” Luba Milambe added. “As we continue the work to increase access to daily oral PrEP, and plan for regulatory review and introduction of the Dapivirine Vaginal Ring, today’s exciting news on cabotegravir brings us another step closer to ensuring more real choice for effective HIV prevention.”

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Press Release

Treatment Action Group and AVAC Statement on Pfizer/BioNTech COVID-19 Vaccine Efficacy Announcement

Treatment Action Group and AVAC Statement on Pfizer/BioNTech COVID-19 Vaccine Efficacy Announcement
Preliminary results suggest the strategy of immunizing with the SARS-CoV-2 spike protein is efficacious, but details are lacking, and the exact nature and duration of the effect is unclear

Contact

Richard Jefferys: richard.jefferys@treatmentactiongroup.org
Kay Marshall, +1 (347) 249-6375, kay@avac.org

New York City, November 9, 2020 — Treatment Action Group (TAG) and AVAC welcome today’s announcement that preliminary data from the efficacy trial of Pfizer/BioNTech’s mRNA COVID-19 vaccine indicates a high-level of protection against COVID-19. Our organizations urge caution, however, given the very limited information that is available only through a company press release.

The manufacturers have reported that greater than 90Ω protection was observed in a preliminary, pre-scheduled assessment of confirmed COVID-19 cases that occurred at least seven days after trial participants received the second injection of the two-dose vaccine regimen. A total of 94 cases of confirmed COVID-19 were included in the analysis, suggesting that nine or fewer were among recipients of the vaccine.

The information was disclosed after an interim analysis by the trial’s Data Safety Monitoring Board (DSMB) and no further details or data were provided (according to reporting by STAT News, even the companies are not privy to additional information). No serious safety issues have been documented to date, but a thorough, independent review of all adverse events will be necessary prior to any marketing of the product. The DSMB has recommended that the trial continue as planned and the final efficacy analysis will be performed after 164 confirmed COVID-19 cases, which may become possible before the end of the year.

The US Food and Drug Administration (FDA) has requested at least two months of safety follow up after the second vaccination before considering an Emergency Use Authorization (EUA), and Pfizer’s CEO Albert Bourla said sufficient safety data to meet this requirement should be available by the third week of November. This is a bare minimum for any review, and TAG and AVAC call for these data to be evaluated by the FDA’s Vaccines and Related Biological Products Advisory Committee (VRBPAC) in December before any action is taken. At the recent VRBPAC meeting on October 22, several members expressed concerns about the implications of vaccine EUAs and suggested that expanded access programs would be a preferable means of providing emergency access prior to full approval.

The Pfizer/BioNTech vaccine is designed to induce immune responses against the SARS-CoV-2 spike protein, a strategy that is also employed by many other candidates that are in efficacy trials. This provides some cause for optimism that multiple other vaccines will prove efficacious.

However, many questions remain given the lack of details available. Pfizer/BioNTech must be maximally transparent in releasing full information and data sets from the trial as they become available. Among the issues that will need to be addressed:

The exact details of the numbers involved, endpoints analyzed, and statistical findings including confidence intervals and p-values;
Efficacy against the range of possible COVID-19 outcomes, from asymptomatic (but potentially transmissible) SARS-CoV-2 infections to severe COVID-19 disease;
Efficacy across diverse populations, particularly those most vulnerable to severe COVID-19 such as the elderly and those with health conditions that may make COVID-19 outcomes worse;
Efficacy in populations that have been omitted from most studies to date, including children and pregnant women;
Full characterization of the safety profile;
Identification of correlates of vaccine-induce immune protection (such as antibody responses);
Investigations into why vaccination did not work in the study participants who acquired COVID-19;
Duration of protection. Studies suggest that immunity to seasonal cold-causing coronaviruses is typically short-lived (~6 months to a year), and it will be important to conduct long-term follow up to learn whether regular re-vaccination may be necessary;
Equitable vaccine distribution in the United States and globally. Factors that will need to be considered include cost, pace of production, availability of supply, and logistical considerations such as refrigeration (the Pfizer/BioNTech mRNA vaccine needs to be stored at -80° C until just before administration);
Ensuring any EUA (if deemed more appropriate than expanded access by FDA) places specific requirements for continued data collection and clearly articulates the pathway and timeline for a full application for licensure; and,
Implications for efficacy trials of other candidates, given that it may become inappropriate for participants to continue to receive placebos if an effective vaccine is available.

Today’s news offers hope that it will be possible to quell the COVID-19 pandemic with vaccination campaigns backed by strong public health measures. However, the data are still preliminary, and a safe, effective, and equitably delivered vaccine will require a great deal more verified, peer-reviewed data and regulatory decisions. Once a vaccine is available, equitable access depends on political will in the form of evidence-based messages, fully funded vaccination campaigns in all countries and communities, and a globally coordinated effort to ensure that supply and demand reflect need, not greed or nationalist responses. TAG and AVAC support the call for a people’s vaccine to made universally available to all at no cost.

TAG and AVAC are heartened by the news of the incoming US administration’s plans for dealing with the COVID pandemic and commend them for the decision to rejoin the World Health Organization (WHO) as soon as possible. We urge them to join multilateral efforts to ensure equitable global allocation and distribution of COVID-19 vaccines. No country in the world, including the United States, will end this pandemic with isolationist responses. The fact that the first report of COVID-19 vaccine efficacy emerged from a collaboration between a German and US company (the former founded by Turkish immigrants; the latter founded by German immigrants) underscores this point.

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Press Release

Global AIDS Policy Partnership Statement in Support of Heroes Act 2020

Contact

Kay Marshall, +1 (347) 249-6375, kay@avac.org

The Global AIDS Policy Partners (GAPP) issued the following statement regarding the Health and Economic Recovery Omnibus Emergency Solutions Act, or Heroes Act, released today:

The Global AIDS Policy Partnership (GAPP) applauds and strongly supports the provision of much-needed funding to global health efforts as part of the next COVID-19 relief package, led by the House Appropriations Committee Chairwoman Nita Lowey and House Speaker Nancy Pelosi.

Including at least $3.5 billion for the Global Fund to Fight AIDS, Tuberculosis and Malaria (GFTAM) to support low to middle income countries to bolster health systems and respond to the outbreak, and $1 billion for the President’s Emergency Plan For AIDS Relief (PEPFAR), will be essential to advance COVID-19-related support for these programs and to resume pre-pandemic work addressing the full array of challenges that these programs now face.

The COVID-19 pandemic has harmed efforts to control HIV and other global health programs and could reverse a decade of progress. In fact, according to UNAIDS, just a six-month disruption in HIV treatment access could lead to an additional 500,000 HIV-related deaths in sub-Saharan Africa alone. We are in the early stages of this new pandemic but have already seen the effects on these other long-standing epidemics. TB case detection programs have stalled in many countries; PEPFAR programs have had to adapt or have halted prevention programming; a number of HIV treatment centers have reported fewer people are accessing antiretroviral treatment raising the threat of greater mortality and HIV infection; and some malaria campaigns have been suspended.

Years of sustained PEPFAR and GFTAM investment has strengthened supported countries’ laboratory networks, surveillance capacity, health care workers and supply chains, allowing them to respond efficiently and effectively to COVID-19. But capacity has become strained as the need to fight both epidemics simultaneously takes hold. While this represents a critical investment in addressing the primary and secondary effects of the COVID-19 pandemic and the resulting recession, much more is and will be needed in the months to come in order to preserve decades of US investments in global health and economic development globally.

Funding allocated in the Heroes Act would allow us to safeguard decades of progress against HIV, TB and malaria and save millions more people from these diseases. This additional funding for the global response to COVID-19 will protect the more than $80 billion investment United States taxpayers have made in stopping three of the world’s most pernicious killers, while allowing the programs designed to combat HIV, TB and malaria to support the response to COVID-19.

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The GAPP is a coalition of over 60 advocacy and implementing organizations committed to expanding and improving global HIV/AIDS programming.

Press Release

AVAC Applauds Positive Opinion from EMA on Woman-initiated Prevention Option

Calls for accelerated implementation research, WHO guidance and
regulatory review for Dapivirine Vaginal Ring

Contact

Mitchell Warren, +1 (914) 661-1536, mitchell@avac.org
Kay Marshall, +1 (347) 249-6375, kay@avac.org

New York City, July 24, 2020 – AVAC applauded the positive opinion adopted today by the European Medicines Agency (EMA) on the use of the Dapivirine Vaginal Ring as an HIV prevention option for cisgender women 18 and older. The International Partnership for Microbicides (IPM), the developer of the ring, announced that it will be moving swiftly toward the next steps needed to get this critical prevention option into the hands of women who want and need it. AVAC congratulates IPM, welcomes this commitment to bringing a much-needed woman-initiated HIV prevention option to women, especially in Eastern and Southern Africa, and calls for an integrated introduction plan that lifts up the voices of women, speeds regulatory approvals and is fully funded.

The Dapivirine Vaginal Ring is a flexible, silicone ring that a woman can insert in the vagina for monthly protection against HIV. It contains the antiretroviral drug dapivirine and is designed to provide women with a discreet and long-acting option for HIV prevention. The ring was shown to be modestly effective in two large efficacy studies and open-label extension studies showed a trend toward higher efficacy when women knew the product they were using contained the active drug.

The EMA’s positive opinion recommends the Dapiviring Vaginal Ring “in combination with safer sex practices when oral pre-exposure prophylaxis (PrEP) is not used, cannot be used or is not available.” This regulatory opinion, generated through a mechanism that allows review of medicines intended for use outside of the EU, triggers critical actions from WHO, including reviewing its HIV treatment and prevention guidelines for possible inclusion of the ring and beginning the pre-qualification process that would help ensure countries are able to approve and procure rings for their programs.

“This is a long-awaited day for the thousands of women in Africa, Europe and the US, who participated in clinical trials of the ring and those of us who have advocated for access to the ring and other women-initiated prevention options for over two decades. Women have been waiting for additional HIV prevention options that they can use discreetly and easily, and for many the ring could be that product,” said Manju Chatani-Gada, AVAC’s Director of Partnerships & Capacity Strengthening. “We’re looking forward to ensuring that women guide and lead the next steps, working with IPM, WHO and country stakeholders to ensure that former trial participants, future users of the ring and women’s health advocates are included in decision-making processes for research and introduction going forward.”

“As a young woman and a youth advocate, I’m so excited by this news. We need diverse prevention options that will meet our needs where we are in our lives. The ring gives us another choice and that’s so important,” said Cleopatra Sheilla Makura, Youth Prevention Advocate and former AVAC Fellow from Zimbabwe. “I can’t wait to share this news with other young women and help plan for the introduction of this new prevention option in our communities.

As part of the opinion, the EMA asked that additional data from cisgender women ages 18-25 be collected to better understand the ring’s efficacy overall and among this group that is often at a higher risk for HIV. They have also asked for more data to be gathered on potential drug resistance among ring users who might become infected. These additional data would complement information from introduction activities that will help program implementers and policy makers better understand how the ring can be effectively provided to women. These early introduction activities will also provide critical data to support integrating the ring into existing HIV prevention programs and sexual and reproductive health programs.

“The positive EMA opinion is a critically important step that helps move the Dapivirine Vaginal Ring from a research product to a reality in women’s lives, and ultimately to public health impact.” said Mitchell Warren, AVAC Executive Director. “AVAC has been proudly working with IPM and a range of other partners to develop a robust plan for ring introduction and scale-up. Now is the time to design and fund strategic introduction of the ring in communities where we know women have been waiting for new HIV prevention options.”

Despite years of expanded treatment and prevention options for HIV, women – especially young women – in many communities remain at substantial risk of HIV infection. Incidence rates in women have remained persistently high at four percent as seen in the MIRA trial thirteen years ago to the ECHO study in 2019 and the recently stopped HVTN 702 vaccine trial earlier this year. Women need and deserve more options from which to choose to protect themselves from HIV.

“The high rates of HIV infection in many communities in East and Southern Africa are a reminder that we have no time to lose,” Warren added. “The US government, several European governments and the Bill & Melinda Gates Foundation have made critical long-term investments in IPM to develop the ring; now these and additional funders need to double down on this initial support to work with IPM and others in the field to ensure the ultimate return on these investments: HIV infections averted. This includes investing in a suite of access activities as well as supporting plans for rapid regulatory review and integration of the ring into existing HIV prevention and SRH programs.”

IPM estimates that the ring could become available in 2021 in some countries in East and Southern Africa. AVAC will continue to work with IPM and other partners through a new consortium – PROMISE – that is supported by USAID and PEPFAR to ensure that the critical next steps, including pilot introduction initiatives that will help guide eventual rollout plans for the ring, continue at pace with plans adapted to meet the current challenges presented by the COVID-19 pandemic.

Additional studies that are ongoing or planned are looking at the safety and acceptability of the ring among young women ages 16 to 21 and women who are pregnant or breastfeeding. The COVID-19 pandemic has slowed some of these studies, but are critical to provide data to help ensure more women will soon have access to the ring

“While the ring is not yet available, we must not forget that highly effective prevention options for women already exist and must be made available: daily oral PrEP and the female condom. Work must continue to expand these options today to strengthen programmatic platforms so that the ring and other future options are rapidly and seamlessly integrated into SRHR services and to enable women to have informed choice among an array of options,” added Chatani-Gada.

In addition, research for additional women-initiated HIV prevention options must be prioritized. Results may come later this year or in 2021 from a trial looking at long-acting injectable PrEP for women and there are multiple other products, some combined with pregnancy prevention, in the pipeline. IPM and partners are testing a Dapivirine Vaginal Ring that would last three months and early stage research of multiple combination HIV prevention and contraceptive products are underway. It is critical that this research continue to be prioritized and fully funded.

More information on the Dapivirine Vaginal Ring is here and here.

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About AVAC: Founded in 1995, AVAC is a non-profit organization that uses education, policy analysis, advocacy and a network of global collaborations to accelerate the ethical development and global delivery of HIV prevention options as part of a comprehensive response to the pandemic.

Press Release

Injectable PrEP is Highly Effective for Some Populations and Must Move Forward as Quickly as Possible

AVAC calls for intensified efforts to increase access to daily oral PrEP

Contact

Mitchell Warren, +1 (914) 661-1536, mitchell@avac.org
Kay Marshall, +1 (347) 249-6375, kay@avac.org

New York City, July 7, 2020 – AVAC welcomes new, additional data that shows an injectable antiretroviral for HIV pre-exposure prophylaxis (PrEP) is safe and highly effective in reducing HIV risk cisgender men and transgender women who have sex with men. At the 23rd International AIDS Conference today researchers from the HIV Prevention Trials Network (HPTN) released data comparing rates of HIV among trial participants who received the bi-monthly injection, and those who received daily oral tenofovir/emtricitabine (TDF/FTC). While both strategies reduced HIV risk among participants, the injectable strategy was more effective compared to oral PrEP.

The overall number of infections in both arms of the study was very low, underscoring the high efficacy of both interventions. Importantly, daily oral PrEP is licensed and available now for men, women and adolescents in many communities around the world.

“It’s great to see such a high level of efficacy in a potential additional HIV prevention option and to see the high level of efficacy for an already available option, daily oral PrEP,” said Mitchell Warren, AVAC Executive Director. “As we celebrate this exciting new data, we also must ensure that the companion HPTN 084 study of the same product in cisgender women finishes as quickly as possible and simultaneously work to ensure broader access and support for daily oral PrEP in communities where it is needed now.”

These data add insight to the May 2020 announcement from HPTN 083 that injectable PrEP was highly-effective. Importantly, investigators shared data on adherence among participants taking oral PrEP and found that 76 percent of a random sample had blood levels consistent with daily use. While additional work to understand the results is ongoing, this suggests that the difference in impact might be due to the products. Use of the injection requires an oral “lead-in” phase, and 48 weeks of oral PrEP use after discontinuation. Learning more about preferences and feasibility of both injectable and oral PrEP among people at risk of HIV is a critical next step.

“We need options that will work in people’s lives, we need existing daily PrEP delivered at scale now, and we need multiple additional PrEP options to address diverse needs. CAB-LA, the dapivirine vaginal ring, and future products that show efficacy must be brought to market as quickly as possible,” added Warren.

Given that current data show efficacy in men who have sex with men and transgender women, but not in cisgender women, where rates in adolescent girls and young women are persistently high, messages, licensure and introduction plans need to be swift, clear and strategic with respect to the growing array of PrEP options available for different groups. ViiV, the manufacturer of CAB-LA, must now move quickly to work with regulatory agencies, to share, for community review and input, its plans for seeking review and the timeline for incorporating data from the ongoing HPTN 084 study, while WHO must simultaneously launch a parallel consultative process to support guidance for CAB-LA, so there will be no delay in rolling the drug out.

In 2018, AVAC and the Clinton Health Access Initiative (CHAI) established the Biomedical Prevention Implementation Collaborative (BioPIC) to work with a wide range of stakeholders to develop an introduction plan for long-acting injectables and other next-generation HIV prevention options. Today’s announcement makes planning all the more important if promising research results are to be translated into public health impact.

“Planning for health systems to meet future demands for a drug delivered by injection every two months must also be prioritized,” said Jessica Rodrigues, AVAC’s Director of Product Introduction and Access. “Daily oral PrEP was proven effective more than a decade ago, yet people who want and need this vital prevention option are still unable to access it in many communities. We must not repeat that cycle with new prevention options like CAB-LA and the monthly dapivirine vaginal ring for women, which is currently under regulatory review.”

These clinical trials are an important step in the process, but much additional work is needed. Every product has unique attributes and challenges, and there is much more to be understood about CAB-LA and the way in which it might be effectively delivered in communities and among populations where it is most needed. The HPTN 083 team is still analyzing the safety data on the oral lead-in period as well as the potential need for oral PrEP to “cover the tail” of participants who wish to stop receiving CAB-LA. The research to date suggests that stopping CAB-LA and clearing the drug from the body may not be as easy as stopping daily oral PrEP, since traces of CAB-LA can linger in the body well after discontinuing injections. It will be essential to understand how this can be addressed outside of a clinical trial setting.

“Understanding the potential risk of drug resistance, user preferences, health system capacity needs, the price of the product and the programs to deliver it and support use, amongst other issues, are necessary to move forward as quickly as possible if the product is ultimately approved for use,” said Rodrigues. “AVAC and our partners have already begun this work and have valuable insights; it now needs to accelerate with global collaboration so that the delays that have slowed the rollout of daily oral PrEP do not recur again.”

Also at AIDS 2020, the SEARCH study presented additional information on the impact of oral PrEP in the context of a comprehensive “health-fair” based approach. SEARCH previously found that this approach, which provided ‘universal testing’ and same-day antiretroviral treatment, reduced incidence by about 30 percent. In the latest data, the SEARCH team found that once daily-oral PrEP was offered to SEARCH participants, new HIV infections dropped by about 75 percent, compared to the period when PrEP was not yet available. This underscores the feasibility and urgency of making oral PrEP a part of comprehensive programs, anchored in a universal testing approach.

“The UNAIDS report and much of the news at this conference is reminding us that the world was failing at HIV prevention before the COVID-19 pandemic hit. SEARCH shows us the possibilities for PrEP success in some of the hardest hit communities in East Africa,” Warren said. “It’s critical that we find ways to scale up innovative daily oral PrEP programs even as we plan for access to new HIV prevention options. We can’t afford any more delays.”

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Press Release

Global Health and Human Rights Organizations Say US Withdrawal from WHO is Reckless Act that Could Delay Americans’ Access to COVID-19 Solutions and Prolong Global Pandemic

Contact

Kay Marshall, +1 (347) 249-6375, kay@avac.org
Suraj Madoori, +1 (917) 530-5996, suraj.madoori@treatmentactiongroup.org
Jessica Bassett, +1 (518) 593-7628, jessica@healthgap.org

New York City, July 7, 2020 – AVAC, Health GAP and the Treatment Action Group (TAG) strongly condemn the Trump Administration’s withdrawal from the World Health Organization (WHO). Today’s announcement formalizing the President’s threats from earlier this year is short-sighted and dangerous, and will cost more lives and deepen economic devastation in the United States and around the world, which are already reeling from the ongoing COVID-19 pandemic.

“This virus respects no borders; COVID-19 anywhere can quickly become COVID-19 everywhere. Global health emergencies require global leadership, and that requires a strong and supported World Health Organization,” said Mitchell Warren, AVAC’s Executive Director. “The Administration is playing politics with people’s lives here in the US and around the world. We will be left behind as the world comes together to collaborate and coordinate science as the best strategy to counter the pandemic, and we will lose ground in our historical investments to end HIV, TB, hepatitis C and other health issues.”

The COVID-19 pandemic has brought unprecedented global cooperation among researchers and funders, with WHO playing a critical role in coordinating both the overall global response and many of the global research initiatives. Global cooperation on public health policy, science, data and information sharing is needed more urgently than ever before. The Trump administration makes a dangerous gamble in thinking that the US can act alone in the response to COVID-19.

“We are seeing the disastrous effects of the US federal government’s lack of strategy playing out every day in increased COVID cases and deaths of Americans, particularly in the Black community,” says Suraj Madoori, TAG’s US and Global Health Policy Director. “Withdrawal from WHO will only compound the issues for our nation and for the world by further retreating on shared responsibilities in public health governance.”

The COVID-19 epidemic is devastating already constrained health systems in low- and middle-income countries where COVID-19 is surging, and has further weakened the US healthcare system as well. At the same time, this new pandemic is already having profound implications on responses to HIV/AIDS, TB, viral hepatitis, malaria, vaccination and contraceptive programs and all other public health responses.

WHO plays a key role in coordination, guidance development and mobilization of these public health responses in countries struggling with COVID-19 in addition to limited resources, conflict and other humanitarian and ecological disaster-related crises. As governments and stakeholders position resources against COVID-19, the WHO has taken the lead in forming the Access to COVID-19 Tools (ACT) Accelerator, a new and needed global collaboration to accelerate development, production and equitable access to COVID-19 tests, treatments and vaccines.

The US, as a historic leader and funder of global public health initiatives, and the largest funder of WHO, has a moral responsibility to help ensure an equitable global response to the COVID-19 pandemic. Terminating the US relationship with WHO starves the organization of funding, US staff and US expertise. It likely prolongs the pandemic and will force WHO to cut critical funding and support for other health programs, including those responding to HIV/AIDS, TB, viral hepatitis, and sexual and reproductive health.

“The Trump administration is shameless in its extreme nationalism at the expense of people’s lives. The WHO performs a vital role in getting new HIV treatments to people around the world safely and quickly and providing key technical assistance to strengthen health systems in vulnerable countries. Trump pulling the US out of the WHO is yet another demonstration of his disregard for people living with HIV around the world,” said Matthew Rose, Director of US Policy and Advocacy for Health GAP.

AVAC, Health GAP and TAG call for the Trump Administration to immediately reverse this disastrous decision, restore and protect funding to WHO and work to ensure global cooperation in the pandemic response.

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About TAG: Treatment Action Group (TAG) is an independent, activist and community-based research and policy think tank fighting for better treatment, prevention, a vaccine and a cure for HIV, tuberculosis and hepatitis C virus. TAG works to ensure that all people with HIV, TB and HCV receive lifesaving treatment, care and information. We are science-based treatment activists working to expand and accelerate vital research and effective community engagement with research and policy institutions.

About Health GAP: Health GAP is an international advocacy organization dedicated to ensuring that all people living with HIV have access to affordable life sustaining medicines. Our team pairs pragmatic policy work with audacious grassroots action to win equitable access to treatment, care and prevention for people living with and affected by HIV worldwide. We are dedicated to eliminating barriers to universal access to affordable life sustaining medicines for people living with HIV/AIDS as key to a comprehensive strategy to confront and ultimately stop the AIDS pandemic. We believe that the human right to life and to health must prevail over the pharmaceutical industry’s excessive profits and expanding patent rights.

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