Efficacy, safety, bone and metabolic effects of HIV nucleoside reverse transcriptase inhibitor BMS-986001 (AI467003): a phase 2b randomised, controlled, partly blinded trial

Gupta, Samir K.; McComsey, Grace A.; Lombaard, John; Echevarría, Juan; Orrell, Catherine; Avihingsanon, Anchalee; Osiyemi, Olayemi; Santoscoy, Mario; Ray, Neelanjana; Stock, David A.; Joshi, Samit R; Hanna, George J.; Lataillade, Max

doi:10.1016/s2352-3018(15)00231-3

Cited by 12 publications

(8 citation statements)

References 26 publications

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“…Ultimately, we included 25 distinct papers for final data extraction (Figure 1). Of these, 10 investigated PrEP users [1,3,11,12,15–20] and were included in our primary analyses, while 15 investigated HIV [21–35]. We did not find any HBV studies or new relevant conference proceedings that had not already been published as one of our reviewed studies.…”

Section: Resultsmentioning

confidence: 99%

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The Effect of Tenofovir Disoproxil Fumarate on Bone Mineral Density: A Systematic Review and Meta-Analysis

et al. 2020

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Background We conducted a systematic review and meta-analysis (CRD#42017070552) to quantify the impact of oral tenofovir disoproxil fumarate/emtricitabine (TDF/FTC) on bone mineral density (BMD) and the risk of osteoporosis, low bone mass and fractures, among people taking it as pre-exposure prophylaxis (PrEP), HIV treatment and HBV treatment. Methods We searched MEDLINE and EMBASE for randomized controlled trials published from 1997–2018 reporting BMD, osteoporosis, low bone mass and/or fractures in treatment-naive patients taking compared with not taking TDF for 48 ±4 weeks. We pooled outcomes using DerSimonian random-effects models. Results Our search yielded 5,178 abstracts, representing 3,865 articles, with 25 meeting the inclusion criteria. TDF was associated with greater BMD decline when taken as PrEP (lumbar spine: mean difference [MD]=-0.82%, 95% CI=-1.28, -0.37%, I2=38%; total hip: MD=-0.81%, 95% CI=-1.22, -0.40%, I2=48%) and HIV treatment (lumbar spine: MD=-1.62%, 95% CI=-2.30, -0.95%, I2=93%; total hip: MD=-1.75%, 95% CI=-2.08, -1.42%, I2=83%; femoral neck: MD=-1.26%, 95% CI=-2.15, -0.38%, I2=43%) in comparison to those not taking TDF. Eight studies reported on incident osteoporosis or low bone mass, with variable results. Pooled results from five PrEP studies showed that TDF was not associated with increased fractures compared with no PrEP (RR=1.12, 95% CI=0.752, 1.74, I2=26%). Conclusions TDF caused greater decreases in BMD than did comparators when used for all three indications and the magnitude of this decrease was larger for HIV treatment compared with PrEP. Fractures were not increased among PrEP patients. The clinically significant BMD decline caused by TDF and current expansion of PrEP use suggest attention to the adverse bone effects of TDF will increase in importance.

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Section: Resultsmentioning

confidence: 99%

“…Nine studies [23,24,26–28,31–34] measured BMD changes over 1 year in people using TDF for HIV. As for the PrEP studies, all showed a larger decrease from baseline in TDF compared with non-TDF treated participants.…”

Section: Resultsmentioning

confidence: 99%

The Effect of Tenofovir Disoproxil Fumarate on Bone Mineral Density: A Systematic Review and Meta-Analysis

et al. 2020

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“…Although d4T itself is being phased out as a treatment for HIV, chemically modified versions of d4T may yet find a place in the future. A 4′‐ethynyl derivative of d4T (BMS‐986001) in Phase 2 trials showed similar efficacy as tenofovir disoproxil fumarate; however, development was discontinued due to a lower resistance barrier and gains in both peripheral and central fat accumulation . Such modifications could add specificity while retaining the flat ring that may allow d4TTP to retain the same catalytic efficiency as dTTP, despite the absence of the 2′ hydroxyl.…”

Section: Discussionmentioning

confidence: 99%

Structure of HIV‐1 reverse transcriptase/d4TTP complex: Novel DNA cross‐linking site and pH‐dependent conformational changes

et al. 2018

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Stavudine (d4T, 2′,3′‐didehydro‐2′,3′‐dideoxythymidine) was one of the first chain‐terminating nucleoside analogs used to treat HIV infection. We present the first structure of the active, triphosphate form of d4T (d4TTP) bound to a catalytic complex of HIV‐1 RT/dsDNA template‐primer. We also present a new strategy for disulfide (S–S) chemical cross‐linking between N6 of a modified adenine at the second overhang base to I63C in the fingers subdomain of RT. The cross‐link site is upstream of the duplex‐binding region of RT, however, the structure is very similar to published RT structures with cross‐linking to Q258C in the thumb, which suggests that cross‐linking at either site does not appreciably perturb the RT/DNA structures. RT has a catalytic maximum at pH 7.5. We determined the X‐ray structures of the I63C‐RT/dsDNA/d4TTP cross‐linked complexes at pH 7, 7.5, 8, 8.5, 9, and 9.5. We found small (~0.5 Å), pH‐dependent motions of the fingers subdomain that folds in to form the dNTP‐binding pocket. We propose that the pH‐activity profile of RT relates to this motion of the fingers. Due to side effects of neuropathy and lipodystrophy, use of d4T has been stopped in most countries, however, chemical modification of d4T might lead to the development of a new class of nucleoside analogs targeting RNA and DNA polymerases.

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“…An ongoing phase 2a study is evaluating the safety and tolerability of TPN-101 on a small sample (40 participants) of C9orf72 ALS/FTD patients (NCT04993755). TPN-101 (OBP-601, BMS-986001, festinavir, censavudine;Smith et al, 2015) is a thymidine analog NRTI (nucleoside reverse transcriptase inhibitor) that shows major efficacy against HIV-2 and HIV-1 (Gupta et al, 2016). The active form of TPN-101 (BMS-986001-5 -triphosphate) is a substrate for incorporation by HIV-1 reverse transcriptase, inducing the termination of viral DNA synthesis (Smith et al, 2015).…”

Section: Tpn-101mentioning

confidence: 99%

C9orf72-Related Neurodegenerative Diseases: From Clinical Diagnosis to Therapeutic Strategies

Zampatti

Peconi

Campopiano

et al. 2022

Front. Aging Neurosci.

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Hexanucleotide expansion in C9orf72 has been related to several phenotypes to date, complicating the clinical recognition of these neurodegenerative disorders. An early diagnosis can improve the management of patients, promoting early administration of therapeutic supportive strategies. Here, we report known clinical presentations of C9orf72-related neurodegenerative disorders, pointing out suggestive phenotypes that can benefit the genetic characterization of patients. Considering the high variability of C9orf72-related disorder, frequent and rare manifestations are described, with detailed clinical, instrumental evaluation, and supportive therapeutical approaches. Furthermore, to improve the understanding of molecular pathways of the disease and potential therapeutical targets, a detailed description of the cellular mechanisms related to the pathological effect of C9orf72 is reported. New promising therapeutical strategies and ongoing studies are reported highlighting their molecular role in cellular pathological pathways of C9orf72. These therapeutic approaches are particularly promising because they seem to stop the disease before neuronal damage. The knowledge of clinical and molecular features of C9orf72-related neurodegenerative disorders improves the therapeutical application of known strategies and will lay the basis for the development of new potential therapies.

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Efficacy, safety, bone and metabolic effects of HIV nucleoside reverse transcriptase inhibitor BMS-986001 (AI467003): a phase 2b randomised, controlled, partly blinded trial

Cited by 12 publications

References 26 publications

The Effect of Tenofovir Disoproxil Fumarate on Bone Mineral Density: A Systematic Review and Meta-Analysis

The Effect of Tenofovir Disoproxil Fumarate on Bone Mineral Density: A Systematic Review and Meta-Analysis

Structure of HIV‐1 reverse transcriptase/d4TTP complex: Novel DNA cross‐linking site and pH‐dependent conformational changes

C9orf72-Related Neurodegenerative Diseases: From Clinical Diagnosis to Therapeutic Strategies

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