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CROI 2015: Tenofovir Alafenamide as Effective but Safer for Kidneys and Bones than TDF
Print Email Details Category: Experimental HIV Drugs Published on Friday, 27 February 2015 00:00 Written by Liz Highleyman
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Paul Sax (Photo: Liz Highleyman)
Tenofovir alafenamide (TAF), a new formulation that has lower concentrations in the blood but reaches higher levels in cells, is as effective as the older version, tenofovir disoproxil fumarate (TDF), according to a report at the 2015 Conference on Retroviruses and Opportunistic Infections (CROI) this week in Seattle. A second study showed that TAF has less detrimental effects on the kidneys and bones compared with TDF. TAF has been submitted for approval in the U.S. and Europe.
Gilead Sciences' tenofovir disoproxil fumarate (Viread) is one of the most widely used antiretroviral drugs. It is a component of the Truvada coformulation -- used for both HIV treatment and pre-exposure prophylaxis (PrEP) -- and of the single-tablet regimens Atripla, Compera, and Stribild. TDF is highly potent and generally safe and well-tolerated, but it can cause kidney and bone toxicity in some patients.
TAF is a new pro-drug that delivers the active agent, tenofovir diphosphate, more efficiently to cells infected with HIV. TAF produces adequate intracellular levels with lower doses, which means lower concentrations in the blood plasma and less drug exposure for the kidneys, bones and other organs and tissues. A Phase 2 clinical trial previously showed that a regimen of TAF plus emtricitabine, elvitegravir, and cobicistat was comparable to TDF/emtricitabine/elvitegravir/cobicistat (Stribild) but caused less kidney impairment and bone loss.
David Wohl from the University of North Carolina presented combined primary results from 2 Phase 3 studies (GS-US-292-0104 and GS-US-292-0111) looking at the antiviral activity and overall safety of TAF in a new single-tablet regimen. Paul Sax from Brigham and Women's Hospital in Boston followed the next day with data on TAF's effects on kidneys, bones, and lipids.
Study 104 and Study 111 were randomized controlled trials conducted in Europe (both), North America (both), Latin America (Study 111), and Asia (Study 104). Together they included 1733 previously untreated participants with similar characteristics in both trials.
Most (85%) were men, one-quarter were black, 19% were Hispanic/Latino, and the median age was 34 years. They had well-controlled HIV disease with a median viral load of 4.58 log copies/mL and a median CD4 cell counts of approximately 400 cells/mm3. They had normal kidney function at baseline with a median estimated glomerular filtration rate (eGFR) of approximately 115 mL/min.
Participants were randomly assigned to receive a once-daily single-tablet regimen containing emtricitabine, elvitegravir, and cobicistat with either 10 mg TAF or 300 mg TDF. The primary analysis was done at week 48 of treatment.
Efficacy and Overall Safety Results
The 2 regimens had similar high efficacy, showing that the TAF coformulation is non-inferior to the TDF coformulation.
At 48 weeks, 92% of people in the TAF arm and 90% in the TDF arm achieved viral suppression (HIV RNA <50 copies/mL) in the combined analysis (93% vs 92% in Study 104; 92% vs 89% in Study 111).
CD4 cell gains were also similar, at 211 cells/mm3 in the TAF arm and 181 cells/mm3 in the TDF arm.
Viral suppression rates for the TAF and TDF regimens were similar regardless of whether participants had high or low baseline viral load, CD4 counts above or below 200 cells/mm3, male or female sex, black or non-black race/ethnicity, and age over or under 50 years.
In both studies, 4% of participants experienced virological failure; among the small number (about 2%) who met the criteria for resistance testing, very few in either arm showed evidence of any primary resistance mutations (0.8% with TAF, 0.6% with TDF).
Treatment was generally safe and well-tolerated and overall drug safety profiles were similar in both arms.
45 patients (5%) in the TAF arm and 71 (8%) in the TDF arm discontinued treatment early, including 8 and 13 people, respectively, who did so due to adverse events.
About 40% of participants overall experienced drug-related adverse events, mostly mild-to-moderate.
The most common side effects were diarrhea (18%), nausea (16%), and headache, all occurring with similar frequency in both groups.
In both the TAF and TDF arms there were few serious adverse events (8% vs 7%) or drug discontinuation for this reason (0.9% vs 1.5%); 20% experienced grade 3 or 4 laboratory abnormalities in both groups.
"Nothing stood out" in terms of adverse events association with TAF that have not already been seen with TDF, Wohl said.
Kidney, Bone, and Lipid Results
In a separate report, Sax described kidney, bone, and lipid-related adverse events and toxicities.
A pharmacokinetic analysis confirmed that TAF produced lower plasma levels of tenofovir than TDF, but intracellular levels were 4 times higher with TAF; the steady-state tenofovir concentration was 91% lower with TAF compared to TDF.
Looking at kidney-related side-effects, eGFR decreased -- indicating worsening function -- by -6.6% in the TAF arm and by -11.2% in the TDF arm by week 48. The change occurred during the first few weeks of treatment and then stabilized.
In the TAF arm there were no kidney-related adverse events leading to treatment discontinuation. 3 people had hypophosphataemia and 2 had protein in their urine. In the TDF arm, there were 4 kidney-related discontinuations: 2 cases of kidney failure, 1 person with decreased eGFR, and 1 with nephropathy. In addition, 1 patient had subclinical tubulopathy, 4 had hypophosphataemia, and 2 each had glucose and protein in their urine. No one in either arm, however, had overt tubulopathy or Fanconi syndrome.
Turning to bone effects, DEXA measurements were done at baseline and at weeks 24 and 48. People taking TAF experienced smaller average decreases in bone mineral density at 48 weeks than people taking TDF at both the spine (-1.30 vs -2.86) and the hip (-0.66 vs -2.95). Spinal bone loss started soon after starting treatment, reaching a plateau at 24 weeks. Hip bone mineral density continued to fall through week 48, but much more steeply in the TDF arm.
However, not everyone experienced bone loss. In the TAF group, 26% had spine bone loss and 17% had hip bone loss of at least 3%. Bone loss occurred more often in the TDF arm, with 45% and 50% having at least a 3% decrease at the spine and hip, respectively. A small proportion of participants actually gained bone density: 7% at both the spine and hip in the TAF arm, and 3% at both sites in the TDF arm.
Finally, researchers looked at blood lipid levels, which are known to play a role in cardiovascular disease. Levels of total, LDL ("bad") and HDL ("good") cholesterol, as well as triglycerides, rose by small amounts across the board, but more so in the TAF arm; total-to-HDL cholesterol ratio stayed about the same.
Sax suggested that the lipid differences might be occurring because tenofovir reduces lipid levels, but the lower concentration produced by TAF does so less compared with TDF.
Conclusions
Wohl’s team concluded that the TAF and TDF coformulations led to "high and similar response rates, irrespective of age, sex, race, HIV-1 RNA, and CD4 cell count," with "low rates of virological failure, with resistance <1% in both arms."
"Efficacy was very comparable and clearly TAF held its own against TDF," Wohl said at a CROI press conference. "This is very reassuring data as we think about TAF as a component of antiretroviral therapy."
Sax’s team concluded that "detailed protocol-specified renal [kidney] and bone endpoints confirmed the favorable safety and tolerability profile of TAF." Compared with TDF, TAF demonstrated no discontinuations due to renal adverse events; significantly smaller decreases in eGFR; significantly less proteinuria, albuminuria, and tubular proteinuria; significantly less impact on spine and hip bone mineral density; and greater increases in fasting lipids.
Sax explained at the press conference that while the long-term clinical effects are not yet known, this analysis "strongly suggests [TAF] will be safer in the long run for the kidneys and bones than TDF."
Based on these favorable findings, Gilead has submitted the TAF coformulation for regulatory review in the U.S. Europe. The U.S. Food and Drug Administration (FDA) is expected to make a decision by November 2015.
Stand-alone TAF is also being developed as a treatment for hepatitis B virus (HBV) infection. In addition, the company is developing a dual coformulation of TAF and emtricitabine, which will be the successor to Truvada.
Asked about the role of TAF as PrEP for HIV prevention, Marshall Fordyce from Gilead said at the press conference that the company is collaborating with the U.S. Centers for Disease Control and Prevention (CDC) on a study of emtricitabine and TAF for PrEP in macaque monkeys. Fordyce noted that the TAF combination "will have the same development pathway" as TDF for PrEP, presumably suggesting that Gilead will not conduct PrEP trials itself. "To reproduce iPrEx [with the new formulation] would be a large undertaking," he |
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