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"description": "Daily Maverick is an independent online news publication and weekly print newspaper in South Africa.\r\n\r\nIt is known for breaking some of the defining stories of South Africa in the past decade, including the Marikana Massacre, in which the South African Police Service killed 34 miners in August 2012.\r\n\r\nIt also investigated the Gupta Leaks, which won the 2019 Global Shining Light Award.\r\n\r\nThat investigation was credited with exposing the Indian-born Gupta family and former President Jacob Zuma for their role in the systemic political corruption referred to as state capture.\r\n\r\nIn 2018, co-founder and editor-in-chief Branislav ‘Branko’ Brkic was awarded the country’s prestigious Nat Nakasa Award, recognised for initiating the investigative collaboration after receiving the hard drive that included the email tranche.\r\n\r\nIn 2021, co-founder and CEO Styli Charalambous also received the award.\r\n\r\nDaily Maverick covers the latest political and news developments in South Africa with breaking news updates, analysis, opinions and more.",
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"contents": "<span style=\"font-weight: 400;\">One of the biggest breakthroughs in HIV treatment in the 1990s came when three different antiretrovirals (ARVs) were used together, suppressing viral replication in multiple ways and preventing the development of drug resistance. Now, trials are showing that certain combinations of just two antiretrovirals might be as good as three, potentially bringing an end to a quarter of a century of triple therapy dominance. </span>\r\n\r\n<span style=\"font-weight: 400;\">The medicines available for the treatment of HIV infection in the public sector in South Africa have changed significantly over the years. But one thing that hasn’t changed is that the standard treatment is made up of three different ARVs – even if they come co-formulated in one pill.</span>\r\n\r\n<span style=\"font-weight: 400;\">The discovery of triple therapy for the treatment of HIV back in the 1990s turned HIV from a death sentence into a manageable disease. The triple was critical, since people who only took one or two ARVs soon developed drug resistance and fell sick again. The idea that you need three ARVs accordingly became one of the cornerstones of HIV treatment for the quarter-century since.</span>\r\n\r\n<span style=\"font-weight: 400;\">But, as discussed at the recent 2021 Southern African HIV Clinicians Society (SAHCS) conference, the era of exclusive triple therapy may be coming to an end as evidence mounts in support of the safety and efficacy of new dual therapy (two-drug) regimens.</span>\r\n\r\n<span style=\"font-weight: 400;\">But why dual therapy if triple therapy is already so good?</span>\r\n\r\n<span style=\"font-weight: 400;\">Speaking at the SAHCS conference, Dr Pedro Cahn, scientific director of the Huesped Foundation in Argentina, acknowledged that the current three-drug regimens are very effective and said that the aim of introducing dual therapy is to make treatment more comfortable for people living with HIV.</span>\r\n\r\n<span style=\"font-weight: 400;\">A dual therapy regimen firstly reduces the drug burden (from three to two), which Cahn said can improve patient adherence and quality of life. He said this can help meet the needs of the ageing HIV population, by reducing antiretroviral exposure, making treatment safer without sacrificing virologic control, as well as reducing drug-drug interactions and costs.</span>\r\n\r\n<span style=\"font-weight: 400;\">Dr Michelle Moorhouse, senior global medical director at the pharmaceutical company ViiV Healthcare, elaborated on the potential benefits of two-drug regimens. </span>\r\n\r\n<span style=\"font-weight: 400;\">“For example, fewer ingredients mean a smaller pill size, which means smaller and lighter packaging,” she said. This can reduce transport and distribution costs, and more stock can be stored in facilities.</span>\r\n\r\n<span style=\"font-weight: 400;\">“Fewer ingredients should also reduce long-term exposure to additional antiretrovirals which may have long-term toxicity… and of course fewer ingredients should also directly reduce costs,” she said.</span>\r\n\r\n<span style=\"font-weight: 400;\">Dual therapy could be particularly beneficial for older people living with HIV. </span>\r\n\r\n<span style=\"font-weight: 400;\">“Management of the older person living with HIV is complex as they often have multiple comorbidities and are at risk of polypharmacy. Two-drug regimens offer exposure to fewer drugs [and] reduced risk of unmanageable drug-drug interactions,” said Moorhouse.</span>\r\n\r\n<b>Evidence for dual therapy</b>\r\n\r\n<span style=\"font-weight: 400;\">Historically, dual therapy has not been as effective as the current three-drug regimens, according to Cahn, but new drug combinations have shown promise in the last few years.</span>\r\n\r\n<span style=\"font-weight: 400;\">During his presentation, Cahn unpacked results from the landmark </span><a href=\"https://www.thelancet.com/journals/lancet/article/PIIS0140-6736(18)32462-0/fulltext\"><span style=\"font-weight: 400;\">Gemini-1 and Gemini-2</span></a><span style=\"font-weight: 400;\"> studies. These were two identical double-blind, randomised, non-inferiority, Phase Three trials that compared a once-daily two-drug regimen of dolutegravir and lamivudine to a once-daily three-drug regimen of dolutegravir, tenofovir disoproxil fumarate, and emtricitabine. The study enrolled patients who had not taken antiretroviral treatment before.</span>\r\n\r\n<span style=\"font-weight: 400;\">According to Cahn, dolutegravir + lamivudine has demonstrated long-term durability and efficiency in patients with high viral load and CD4+ T-cell count of <200 cell/mm3. No treatment-emergent resistance was observed among participants who met virologic withdrawal in the Gemini-1 and Gemini-2 studies at week 48 or week 96, according to Cahn, and the safety and biomarkers generally favoured dolutegravir + lamivudine.</span>\r\n\r\n<span style=\"font-weight: 400;\">The studies also showed that there was a significantly lower risk of drug-related adverse events with the two-drug combination (20%), compared to 27% for the three-drug combination. But a higher mean weight gain of 3.7kg was observed with dual therapy, compared to 2.4kg with triple therapy.</span>\r\n\r\n<span style=\"font-weight: 400;\">While Cahn said that optimal two-drug regimens are potent, convenient, well-tolerated, and have a high barrier to resistance, he also stressed that more research for these regimens needs to be done in pregnant women, children, and people with HIV and TB coinfection.</span>\r\n\r\n<b>Promising two-drug regimens</b>\r\n\r\n<span style=\"font-weight: 400;\">A </span><a href=\"https://link.springer.com/article/10.1007%2Fs40121-020-00290-w\"><span style=\"font-weight: 400;\">systematic review</span></a><span style=\"font-weight: 400;\">, published in 2020 in the </span><i><span style=\"font-weight: 400;\">Infectious Diseases and Therapy </span></i><span style=\"font-weight: 400;\">journal</span><i><span style=\"font-weight: 400;\">,</span></i><span style=\"font-weight: 400;\"> looked at 33 studies conducted on dual therapy, either as an initial treatment option or as a switch option.</span>\r\n\r\n<span style=\"font-weight: 400;\">The review concluded that lamivudine was the most commonly used Nucleoside Reverse Transcriptase Inhibitor in two-drug regimens that “met non-inferiority” in both treatment-naïve and treatment-experienced populations.</span>\r\n\r\n<span style=\"font-weight: 400;\">For now, it seems lamivudine is best paired with the integrase inhibitor dolutegravir, as was done in the Gemini studies.</span>\r\n\r\n<span style=\"font-weight: 400;\">According to the review, dolutegravir + lamivudine is the most promising NRTI-inclusive two-drug regimen for patients initiating antiretroviral therapy, so much so that recent guidelines updates for the European AIDS Clinical Society, as well as the Department of Health and Human Services in the US, recommend that the combination is considered as a treatment option in treatment-naïve patients, except for individuals with viral loads above 500,000 copies/ml, or active hepatitis B virus (HBV) coinfection.</span>\r\n\r\n<span style=\"font-weight: 400;\">According to the review, lamivudine in combination with a boosted protease inhibitor also showed efficacy in treatment naïve patients. For example, the </span><a href=\"https://www.natap.org/2017/IAS/IAS_13.htm\"><span style=\"font-weight: 400;\">Andes</span></a> <span style=\"font-weight: 400;\">and </span><a href=\"https://pubmed.ncbi.nlm.nih.gov/24783988/\"><span style=\"font-weight: 400;\">Gardel</span></a><span style=\"font-weight: 400;\"> studies found that lamivudine + darunavir/ritonavir and lamivudine + lopinavir/ritonavir were non-inferior to three-drug regimens.</span>\r\n\r\n<p><img loading=\"lazy\" class=\"size-full wp-image-1113614\" src=\"https://www.dailymaverick.co.za/wp-content/uploads/2021/12/MC-2or3-Meds.jpg\" alt=\"hiv dual therapy\" width=\"720\" height=\"417\" /> Trials are showing that certain combinations of just two antiretrovirals might be as good as three, potentially bringing an end to a quarter of a century of triple therapy dominance. (Photo: Spotlight)</p>\r\n\r\n<b>Long-acting, injectable dual therapy</b><span style=\"font-weight: 400;\"> </span>\r\n\r\n<span style=\"font-weight: 400;\">While dolutegravir + lamivudine is the front-runner for dual therapy taken as a pill, other combinations are leading the way when it comes to dual therapy taken as a long-acting injection.</span>\r\n\r\n<span style=\"font-weight: 400;\">In her conference presentation, Moorhouse focused on the long-acting injectable combination of cabotegravir and rilpivirine. According to Moorhouse, the </span><a href=\"https://www.nejm.org/doi/full/10.1056/NEJMoa1904398\"><span style=\"font-weight: 400;\">Atlas</span></a><span style=\"font-weight: 400;\"> and</span><a href=\"https://pubmed.ncbi.nlm.nih.gov/34656207/\"><span style=\"font-weight: 400;\"> Flare</span></a><span style=\"font-weight: 400;\"> studies demonstrated that a monthly injection of this combination was non-inferior to daily oral antiretroviral therapy. Preliminary data from the </span><a href=\"https://pubmed.ncbi.nlm.nih.gov/33308425/\"><span style=\"font-weight: 400;\">Atlas 2M</span></a><span style=\"font-weight: 400;\"> study went further to show non-inferiority of two-monthly compared to monthly dosing.</span>\r\n\r\n<span style=\"font-weight: 400;\">Injectable dual therapy consisting of cabotegravir and rilpivirine was </span><a href=\"https://www.fda.gov/drugs/human-immunodeficiency-virus-hiv/fda-approves-cabenuva-and-vocabria-treatment-hiv-1-infection\"><span style=\"font-weight: 400;\">approved</span></a><span style=\"font-weight: 400;\"> by the United States Food and Drug Administration in January 2021. It is not listed as a registered product on the </span><a href=\"https://registered-health-products.sahpra.org.za/\"><span style=\"font-weight: 400;\">website</span></a><span style=\"font-weight: 400;\"> of the South African Health Products Regulatory Authority.</span>\r\n\r\n<b>Challenges in South Africa</b><span style=\"font-weight: 400;\"> </span>\r\n\r\n<span style=\"font-weight: 400;\">While developments in dual therapy are exciting, there are also potential barriers to rolling out two-drug regimens in South Africa, according to Professor Francois Venter, division head of Ezintsha at the University of the Witwatersrand.</span>\r\n\r\n<span style=\"font-weight: 400;\">One concern for Venter is that women, particularly pregnant women, are underrepresented in a lot of studies on new HIV drugs, including studies on two-drug regimens. He says more data for this population is required.</span>\r\n\r\n<span style=\"font-weight: 400;\">Another barrier that can hinder the adoption of dual therapy, particularly the dolutegravir+ lamivudine regimen, is the high prevalence of hepatitis B in the country. </span>\r\n\r\n<span style=\"font-weight: 400;\">“It’s important to understand that in many ways, hepatitis B is the biggest gatekeeper to two drug therapies at the moment, including dolutegravir+ lamivudine,” Venter said.</span>\r\n\r\n<span style=\"font-weight: 400;\">As Moorhouse points out, dolutegravir + lamivudine may treat HIV, but is insufficient to treat hepatitis B. It thus follows that people should be screened for hepatitis B before being started on dual therapy – in the absence of such screening, triple therapy would be a safer option.</span>\r\n\r\n<span style=\"font-weight: 400;\">According to the 2019 </span><a href=\"https://www.nicd.ac.za/wp-content/uploads/2021/08/RSA_NationalHepatitisGuidelines_final_dec_2019.pdf\"><span style=\"font-weight: 400;\">National Guidelines for the Management of Viral Hepatitis</span></a><span style=\"font-weight: 400;\">, hepatitis B “is endemic in South Africa, resulting in a significant burden of clinical disease as a result of the progression to cirrhosis and the development of the complications of liver failure or hepatocellular carcinoma”. </span>\r\n\r\n<span style=\"font-weight: 400;\">Hepatitis B prevalence estimates for South Africa vary widely, with the best evidence suggesting that it is around 6.7% overall, with higher rates in people living with HIV. Tenofovir, which forms part of standard triple therapy HIV treatment in South Africa, is also used to treat hepatitis B.</span>\r\n\r\n<span style=\"font-weight: 400;\">“If we can’t screen for hepatitis B, we can’t use it [dolutegravir + lamivudine]…. I don’t think HIV programmes should be held hostage for the rest of time to the hepatitis B programme,” Venter said. “We do acknowledge that’s important, but it’s not important enough to inform first-line therapies to the detriment of people having access to new and innovative therapies.”</span>\r\n\r\n<b>TB drug interactions</b>\r\n\r\n<span style=\"font-weight: 400;\">Another problem is that rifampicin, a critically important medicine for the treatment of drug-sensitive TB, interacts with many of the drugs found in the current dual therapy HIV regimens.</span>\r\n\r\n<span style=\"font-weight: 400;\">“TB is a constant problem and rifampicin is such a potent driver of drug interactions and it has drug interactions with almost every one of the dual therapy agents we’re looking at at the moment other than lamivudine,” Venter said.</span>\r\n\r\n<span style=\"font-weight: 400;\">Yet, Venter explained that there are excellent first- and second-line treatment options for people living with HIV who also have a TB infection, and those drugs can be used to treat those patients instead of dual therapy regimens. “We have potent drug programmes for these patients and it’s not a deal-breaker any more,” he said.</span>\r\n\r\n<b>Programmatic issues</b>\r\n\r\n<span style=\"font-weight: 400;\">For Venter, the programmatic issues in South Africa are the biggest headache.</span>\r\n\r\n<span style=\"font-weight: 400;\">He explained that while patients are closely monitored and there are follow-ups during clinical trials, patients in the real-world setting in clinics are not followed up as closely. This poses a big problem when rolling out dual therapies, particularly long-acting therapy. If patients miss their appointments for long-acting treatments, this can be disastrous from a resistance perspective.</span>\r\n\r\n<span style=\"font-weight: 400;\">He said that healthcare workers and patients would need to undergo training for using dual therapy, particularly the long-acting injectables. He added that the cost of dual therapies and potential logistical challenges like some long-acting injectable dual therapies requiring cold-chain storage would also need to be considered.</span>\r\n\r\n<span style=\"font-weight: 400;\">Another factor that the government and donors will need to consider, according to Venter, is whether dual therapy will be licensed and if generics will be produced, as this will also affect cost. </span>\r\n\r\n<span style=\"font-weight: 400;\">“We must not underestimate the programmatic issues,” Venter said, “and we must start thinking hard now, starting to put our heads together, start thinking [about getting these] things out to everyone that needs them. Because if it does come, we need to make sure that we’re in a much stronger position to milk the benefits of this new, exciting innovation as quickly as humanly possible in first- and second-line therapy as we go forward.” </span><b>DM/MC</b>\r\n\r\n<em>This article was produced by <a href=\"https://www.spotlightnsp.co.za/2021/12/01/are-two-medicines-instead-of-three-the-future-of-hiv-treatment/\"><span style=\"font-weight: 400;\">Spotlight</span></a> – health journalism in the public interest.</em>\r\n\r\n<img loading=\"lazy\" class=\"aligncenter size-full wp-image-540125\" src=\"https://www.dailymaverick.co.za/wp-content/uploads/spotlight.png\" alt=\"\" width=\"720\" height=\"169\" />\r\n\r\n<i><span style=\"font-weight: 400;\">[hearken id=\"daily-maverick/8881\"]</span></i>",
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"description": "<span style=\"font-weight: 400;\">One of the biggest breakthroughs in HIV treatment in the 1990s came when three different antiretrovirals (ARVs) were used together, suppressing viral replication in multiple ways and preventing the development of drug resistance. Now, trials are showing that certain combinations of just two antiretrovirals might be as good as three, potentially bringing an end to a quarter of a century of triple therapy dominance. </span>\r\n\r\n<span style=\"font-weight: 400;\">The medicines available for the treatment of HIV infection in the public sector in South Africa have changed significantly over the years. But one thing that hasn’t changed is that the standard treatment is made up of three different ARVs – even if they come co-formulated in one pill.</span>\r\n\r\n<span style=\"font-weight: 400;\">The discovery of triple therapy for the treatment of HIV back in the 1990s turned HIV from a death sentence into a manageable disease. The triple was critical, since people who only took one or two ARVs soon developed drug resistance and fell sick again. The idea that you need three ARVs accordingly became one of the cornerstones of HIV treatment for the quarter-century since.</span>\r\n\r\n<span style=\"font-weight: 400;\">But, as discussed at the recent 2021 Southern African HIV Clinicians Society (SAHCS) conference, the era of exclusive triple therapy may be coming to an end as evidence mounts in support of the safety and efficacy of new dual therapy (two-drug) regimens.</span>\r\n\r\n<span style=\"font-weight: 400;\">But why dual therapy if triple therapy is already so good?</span>\r\n\r\n<span style=\"font-weight: 400;\">Speaking at the SAHCS conference, Dr Pedro Cahn, scientific director of the Huesped Foundation in Argentina, acknowledged that the current three-drug regimens are very effective and said that the aim of introducing dual therapy is to make treatment more comfortable for people living with HIV.</span>\r\n\r\n<span style=\"font-weight: 400;\">A dual therapy regimen firstly reduces the drug burden (from three to two), which Cahn said can improve patient adherence and quality of life. He said this can help meet the needs of the ageing HIV population, by reducing antiretroviral exposure, making treatment safer without sacrificing virologic control, as well as reducing drug-drug interactions and costs.</span>\r\n\r\n<span style=\"font-weight: 400;\">Dr Michelle Moorhouse, senior global medical director at the pharmaceutical company ViiV Healthcare, elaborated on the potential benefits of two-drug regimens. </span>\r\n\r\n<span style=\"font-weight: 400;\">“For example, fewer ingredients mean a smaller pill size, which means smaller and lighter packaging,” she said. This can reduce transport and distribution costs, and more stock can be stored in facilities.</span>\r\n\r\n<span style=\"font-weight: 400;\">“Fewer ingredients should also reduce long-term exposure to additional antiretrovirals which may have long-term toxicity… and of course fewer ingredients should also directly reduce costs,” she said.</span>\r\n\r\n<span style=\"font-weight: 400;\">Dual therapy could be particularly beneficial for older people living with HIV. </span>\r\n\r\n<span style=\"font-weight: 400;\">“Management of the older person living with HIV is complex as they often have multiple comorbidities and are at risk of polypharmacy. Two-drug regimens offer exposure to fewer drugs [and] reduced risk of unmanageable drug-drug interactions,” said Moorhouse.</span>\r\n\r\n<b>Evidence for dual therapy</b>\r\n\r\n<span style=\"font-weight: 400;\">Historically, dual therapy has not been as effective as the current three-drug regimens, according to Cahn, but new drug combinations have shown promise in the last few years.</span>\r\n\r\n<span style=\"font-weight: 400;\">During his presentation, Cahn unpacked results from the landmark </span><a href=\"https://www.thelancet.com/journals/lancet/article/PIIS0140-6736(18)32462-0/fulltext\"><span style=\"font-weight: 400;\">Gemini-1 and Gemini-2</span></a><span style=\"font-weight: 400;\"> studies. These were two identical double-blind, randomised, non-inferiority, Phase Three trials that compared a once-daily two-drug regimen of dolutegravir and lamivudine to a once-daily three-drug regimen of dolutegravir, tenofovir disoproxil fumarate, and emtricitabine. The study enrolled patients who had not taken antiretroviral treatment before.</span>\r\n\r\n<span style=\"font-weight: 400;\">According to Cahn, dolutegravir + lamivudine has demonstrated long-term durability and efficiency in patients with high viral load and CD4+ T-cell count of <200 cell/mm3. No treatment-emergent resistance was observed among participants who met virologic withdrawal in the Gemini-1 and Gemini-2 studies at week 48 or week 96, according to Cahn, and the safety and biomarkers generally favoured dolutegravir + lamivudine.</span>\r\n\r\n<span style=\"font-weight: 400;\">The studies also showed that there was a significantly lower risk of drug-related adverse events with the two-drug combination (20%), compared to 27% for the three-drug combination. But a higher mean weight gain of 3.7kg was observed with dual therapy, compared to 2.4kg with triple therapy.</span>\r\n\r\n<span style=\"font-weight: 400;\">While Cahn said that optimal two-drug regimens are potent, convenient, well-tolerated, and have a high barrier to resistance, he also stressed that more research for these regimens needs to be done in pregnant women, children, and people with HIV and TB coinfection.</span>\r\n\r\n<b>Promising two-drug regimens</b>\r\n\r\n<span style=\"font-weight: 400;\">A </span><a href=\"https://link.springer.com/article/10.1007%2Fs40121-020-00290-w\"><span style=\"font-weight: 400;\">systematic review</span></a><span style=\"font-weight: 400;\">, published in 2020 in the </span><i><span style=\"font-weight: 400;\">Infectious Diseases and Therapy </span></i><span style=\"font-weight: 400;\">journal</span><i><span style=\"font-weight: 400;\">,</span></i><span style=\"font-weight: 400;\"> looked at 33 studies conducted on dual therapy, either as an initial treatment option or as a switch option.</span>\r\n\r\n<span style=\"font-weight: 400;\">The review concluded that lamivudine was the most commonly used Nucleoside Reverse Transcriptase Inhibitor in two-drug regimens that “met non-inferiority” in both treatment-naïve and treatment-experienced populations.</span>\r\n\r\n<span style=\"font-weight: 400;\">For now, it seems lamivudine is best paired with the integrase inhibitor dolutegravir, as was done in the Gemini studies.</span>\r\n\r\n<span style=\"font-weight: 400;\">According to the review, dolutegravir + lamivudine is the most promising NRTI-inclusive two-drug regimen for patients initiating antiretroviral therapy, so much so that recent guidelines updates for the European AIDS Clinical Society, as well as the Department of Health and Human Services in the US, recommend that the combination is considered as a treatment option in treatment-naïve patients, except for individuals with viral loads above 500,000 copies/ml, or active hepatitis B virus (HBV) coinfection.</span>\r\n\r\n<span style=\"font-weight: 400;\">According to the review, lamivudine in combination with a boosted protease inhibitor also showed efficacy in treatment naïve patients. For example, the </span><a href=\"https://www.natap.org/2017/IAS/IAS_13.htm\"><span style=\"font-weight: 400;\">Andes</span></a> <span style=\"font-weight: 400;\">and </span><a href=\"https://pubmed.ncbi.nlm.nih.gov/24783988/\"><span style=\"font-weight: 400;\">Gardel</span></a><span style=\"font-weight: 400;\"> studies found that lamivudine + darunavir/ritonavir and lamivudine + lopinavir/ritonavir were non-inferior to three-drug regimens.</span>\r\n\r\n[caption id=\"attachment_1113614\" align=\"aligncenter\" width=\"720\"]<img class=\"size-full wp-image-1113614\" src=\"https://www.dailymaverick.co.za/wp-content/uploads/2021/12/MC-2or3-Meds.jpg\" alt=\"hiv dual therapy\" width=\"720\" height=\"417\" /> Trials are showing that certain combinations of just two antiretrovirals might be as good as three, potentially bringing an end to a quarter of a century of triple therapy dominance. (Photo: Spotlight)[/caption]\r\n\r\n<b>Long-acting, injectable dual therapy</b><span style=\"font-weight: 400;\"> </span>\r\n\r\n<span style=\"font-weight: 400;\">While dolutegravir + lamivudine is the front-runner for dual therapy taken as a pill, other combinations are leading the way when it comes to dual therapy taken as a long-acting injection.</span>\r\n\r\n<span style=\"font-weight: 400;\">In her conference presentation, Moorhouse focused on the long-acting injectable combination of cabotegravir and rilpivirine. According to Moorhouse, the </span><a href=\"https://www.nejm.org/doi/full/10.1056/NEJMoa1904398\"><span style=\"font-weight: 400;\">Atlas</span></a><span style=\"font-weight: 400;\"> and</span><a href=\"https://pubmed.ncbi.nlm.nih.gov/34656207/\"><span style=\"font-weight: 400;\"> Flare</span></a><span style=\"font-weight: 400;\"> studies demonstrated that a monthly injection of this combination was non-inferior to daily oral antiretroviral therapy. Preliminary data from the </span><a href=\"https://pubmed.ncbi.nlm.nih.gov/33308425/\"><span style=\"font-weight: 400;\">Atlas 2M</span></a><span style=\"font-weight: 400;\"> study went further to show non-inferiority of two-monthly compared to monthly dosing.</span>\r\n\r\n<span style=\"font-weight: 400;\">Injectable dual therapy consisting of cabotegravir and rilpivirine was </span><a href=\"https://www.fda.gov/drugs/human-immunodeficiency-virus-hiv/fda-approves-cabenuva-and-vocabria-treatment-hiv-1-infection\"><span style=\"font-weight: 400;\">approved</span></a><span style=\"font-weight: 400;\"> by the United States Food and Drug Administration in January 2021. It is not listed as a registered product on the </span><a href=\"https://registered-health-products.sahpra.org.za/\"><span style=\"font-weight: 400;\">website</span></a><span style=\"font-weight: 400;\"> of the South African Health Products Regulatory Authority.</span>\r\n\r\n<b>Challenges in South Africa</b><span style=\"font-weight: 400;\"> </span>\r\n\r\n<span style=\"font-weight: 400;\">While developments in dual therapy are exciting, there are also potential barriers to rolling out two-drug regimens in South Africa, according to Professor Francois Venter, division head of Ezintsha at the University of the Witwatersrand.</span>\r\n\r\n<span style=\"font-weight: 400;\">One concern for Venter is that women, particularly pregnant women, are underrepresented in a lot of studies on new HIV drugs, including studies on two-drug regimens. He says more data for this population is required.</span>\r\n\r\n<span style=\"font-weight: 400;\">Another barrier that can hinder the adoption of dual therapy, particularly the dolutegravir+ lamivudine regimen, is the high prevalence of hepatitis B in the country. </span>\r\n\r\n<span style=\"font-weight: 400;\">“It’s important to understand that in many ways, hepatitis B is the biggest gatekeeper to two drug therapies at the moment, including dolutegravir+ lamivudine,” Venter said.</span>\r\n\r\n<span style=\"font-weight: 400;\">As Moorhouse points out, dolutegravir + lamivudine may treat HIV, but is insufficient to treat hepatitis B. It thus follows that people should be screened for hepatitis B before being started on dual therapy – in the absence of such screening, triple therapy would be a safer option.</span>\r\n\r\n<span style=\"font-weight: 400;\">According to the 2019 </span><a href=\"https://www.nicd.ac.za/wp-content/uploads/2021/08/RSA_NationalHepatitisGuidelines_final_dec_2019.pdf\"><span style=\"font-weight: 400;\">National Guidelines for the Management of Viral Hepatitis</span></a><span style=\"font-weight: 400;\">, hepatitis B “is endemic in South Africa, resulting in a significant burden of clinical disease as a result of the progression to cirrhosis and the development of the complications of liver failure or hepatocellular carcinoma”. </span>\r\n\r\n<span style=\"font-weight: 400;\">Hepatitis B prevalence estimates for South Africa vary widely, with the best evidence suggesting that it is around 6.7% overall, with higher rates in people living with HIV. Tenofovir, which forms part of standard triple therapy HIV treatment in South Africa, is also used to treat hepatitis B.</span>\r\n\r\n<span style=\"font-weight: 400;\">“If we can’t screen for hepatitis B, we can’t use it [dolutegravir + lamivudine]…. I don’t think HIV programmes should be held hostage for the rest of time to the hepatitis B programme,” Venter said. “We do acknowledge that’s important, but it’s not important enough to inform first-line therapies to the detriment of people having access to new and innovative therapies.”</span>\r\n\r\n<b>TB drug interactions</b>\r\n\r\n<span style=\"font-weight: 400;\">Another problem is that rifampicin, a critically important medicine for the treatment of drug-sensitive TB, interacts with many of the drugs found in the current dual therapy HIV regimens.</span>\r\n\r\n<span style=\"font-weight: 400;\">“TB is a constant problem and rifampicin is such a potent driver of drug interactions and it has drug interactions with almost every one of the dual therapy agents we’re looking at at the moment other than lamivudine,” Venter said.</span>\r\n\r\n<span style=\"font-weight: 400;\">Yet, Venter explained that there are excellent first- and second-line treatment options for people living with HIV who also have a TB infection, and those drugs can be used to treat those patients instead of dual therapy regimens. “We have potent drug programmes for these patients and it’s not a deal-breaker any more,” he said.</span>\r\n\r\n<b>Programmatic issues</b>\r\n\r\n<span style=\"font-weight: 400;\">For Venter, the programmatic issues in South Africa are the biggest headache.</span>\r\n\r\n<span style=\"font-weight: 400;\">He explained that while patients are closely monitored and there are follow-ups during clinical trials, patients in the real-world setting in clinics are not followed up as closely. This poses a big problem when rolling out dual therapies, particularly long-acting therapy. If patients miss their appointments for long-acting treatments, this can be disastrous from a resistance perspective.</span>\r\n\r\n<span style=\"font-weight: 400;\">He said that healthcare workers and patients would need to undergo training for using dual therapy, particularly the long-acting injectables. He added that the cost of dual therapies and potential logistical challenges like some long-acting injectable dual therapies requiring cold-chain storage would also need to be considered.</span>\r\n\r\n<span style=\"font-weight: 400;\">Another factor that the government and donors will need to consider, according to Venter, is whether dual therapy will be licensed and if generics will be produced, as this will also affect cost. </span>\r\n\r\n<span style=\"font-weight: 400;\">“We must not underestimate the programmatic issues,” Venter said, “and we must start thinking hard now, starting to put our heads together, start thinking [about getting these] things out to everyone that needs them. Because if it does come, we need to make sure that we’re in a much stronger position to milk the benefits of this new, exciting innovation as quickly as humanly possible in first- and second-line therapy as we go forward.” </span><b>DM/MC</b>\r\n\r\n<em>This article was produced by <a href=\"https://www.spotlightnsp.co.za/2021/12/01/are-two-medicines-instead-of-three-the-future-of-hiv-treatment/\"><span style=\"font-weight: 400;\">Spotlight</span></a> – health journalism in the public interest.</em>\r\n\r\n<img class=\"aligncenter size-full wp-image-540125\" src=\"https://www.dailymaverick.co.za/wp-content/uploads/spotlight.png\" alt=\"\" width=\"720\" height=\"169\" />\r\n\r\n<i><span style=\"font-weight: 400;\">[hearken id=\"daily-maverick/8881\"]</span></i>",
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"summary": "The era of exclusive triple therapy for the treatment of HIV may be coming to an end as evidence mounts in support of the safety and efficacy of new dual-therapy (two-drug) regimens.",
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