Pharmacokinetic and Tissue Distribution Profile of Long Acting Tenofovir Alafenamide and Elvitegravir Loaded Nanoparticles in Humanized Mice Model

Prathipati, Pavan Kumar; Mandal, Subhra; Pon, Gregory; Vivekanandan, Renuga; Destache, Christopher J.

doi:10.1007/s11095-017-2255-7

Cited by 31 publications

(16 citation statements)

References 21 publications

(30 reference statements)

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“…The presence of substantially elevated IR fluorescence until the end of study (14 days post-injection) at the injection site and within clearance organs (liver and kidney) indicates at the injection site cARV NPs could act as a "cARV NP depo" inducing sustained NP release. The above observation follows the previous PK studies, reporting high cARVs concentration at the injection site and clearance organs at the terminal time-point (Prathipati et al, 2017).…”

Section: Discussionsupporting

confidence: 91%

“…Previous PK studies suggested that subQ injected cARV NP leads to ARVs target tissue-level significantly above the IC 90 (Mandal et al, 2017a(Mandal et al, , 2017bPrathipati et al, 2017) for all three studied ARVs. Compared to single cARV PK studies (Mandal et al, 2017a(Mandal et al, , 2017bPrathipati et al, 2017), multiple dosage of cARV NPs illustrated even higher tissue ARV levels at 22 week (2 weeks post-terminal dose, Table 2). Further, sustained non-detectable pVL (Fig.…”

Section: Discussionmentioning

confidence: 74%

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Long-acting parenteral combination antiretroviral loaded nano-drug delivery system to treat chronic HIV-1 infection: A humanized mouse model study

et al. 2018

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Human immunodeficiency virus (HIV) patients are often diagnosed in the chronic stage of HIV/AIDS. Combination antiretroviral therapy (cART) has improved quality of life for HIV-infected patients. Present study describes a novel long-acting parenteral formulation of combination antiretroviral (cARV) loaded nano-drugs for treating chronic HIV-1 (cHIV) in a humanized-BLT (hu-BLT) mice model. The cARV (elvitegravir+tenofovir alafenamide+emtricitabine; EVG+TAF+FTC) drugs (mimicking marketed Genvoya one-pill for HIV-treatment) were encapsulated in poly (lactic-co-glycolic acid) nanoparticles (NPs). To establish cHIV, hu-BLT mice were intravaginally challenged with HIV-1 and maintained for 15 weeks. Plasma viral load (pVL) was monitored by RT-PCR to confirm cHIV. Baseline pVL (week 15) was comparable between treated (n = 10) and control (n = 5) mice groups. Subsequently, treatment hu-BLT mice received 3 subcutaneous doses of cARV NPs (417 mg/kg per dose; n = 10), biweekly, and a fourth/terminal dose a week later. Prior to each treatment and on sacrifice (week 24), pVL was determined. Within three subcutaneous doses of cARV NPs, a non-detectable pVL was established (week 19) and continued until week 22. After the establishment of a non-detectable pVL (week 19-22), 4 treated-mice were sacrificed for tissue drug concentration determination by LC-MS/MS analysis. A considerable amount of cARV was detected at the HIV-infection target and reservoir organs. Subsequently, pVL rebounded comparable to control group by week 24, (7 weeks post-terminal dosage). The present study demonstrated cARV NPs augments sustained ARV efficacy in the cHIV humanized-mouse model. Therefore, cARV NPs could be a novel delivery system to treat cHIV patients, by overcoming drawbacks of conventional cART.

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Section: Discussionsupporting

confidence: 91%

Section: Discussionmentioning

confidence: 74%

Long-acting parenteral combination antiretroviral loaded nano-drug delivery system to treat chronic HIV-1 infection: A humanized mouse model study

et al. 2018

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“…BIC loaded NPs (BIC NPs) were formulated using previously reported oil-in-water (o-w) emulsion method with some modifications (Destache et al, 2016;Mandal et al, 2017c;Prathipati et al, 2017). Briefly, the 5 mL DCM (organic phase) containing PLGA, PF-127 (stabilizer) and BIC at 10:10:2 (w:w:w), respectively, was added dropwise to 20 mL of 1% PVA solution (aqueous phase), under high speed continuous stirring condition.…”

Section: Bic Np Formulation and Characterizationmentioning

confidence: 99%

“…Various longacting injectable small molecule ARV agents are already in clinical trials (Spreen et al, 2013). Our research goal is to introduce long-action to conventional ARVs by fabricating single or multiple ARV (combination ARVs, cARVs) in polymeric nanoformulations as a long-acting parenteral drug delivery system for HIV treatment and prevention (Mandal et al, 2017b(Mandal et al, , 2017cPrathipati et al, 2017;Shibata et al, 2013). Our long-acting FTC NPs (Mandal et al, 2017a), TAF+FTC NPs as well as TAF+elvitegravir (EVG) NPs were efficacious as prevention regimens (Mandal et al, 2017b(Mandal et al, , 2017cPrathipati et al, 2017;Shibata et al, 2013), and TAF +FTC+EVG NPs demonstrated efficacy as chronic HIV treatment (Mandal et al, 2018) in humanized mice.…”

Section: Introductionmentioning

confidence: 99%

A potential long-acting bictegravir loaded nano-drug delivery system for HIV-1 infection: A proof-of-concept study

et al. 2019

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Bictegravir (BIC), a newly FDA-approved integrase strand transfer inhibitor (INSTI), as a single tablet regimen has proven efficacious in treating HIV-1 and SIV viruses, with reduced resistance. BIC clinical trials have not investigated its prophylaxis potency. This study investigates the HIV prevention potency of a novel long-acting BIC nano-formulation aimed to improve adherence. Poly (lactic-co-glycolic acid) loaded BIC nanoparticles (BIC NPs) were formulated using an oilin-water emulsion methodology. BIC NPs were < 200 nm in size, with 47.9 ± 6.9% encapsulation efficiency. A novel, sensitive and high throughput LC-MS/MS method was used to estimate intracellular pharmacokinetics (PK) of BIC NPs and compared to BIC solution demonstrated prolonged intracellular BIC retention. BIC NPs safety was assessed based on cytotoxicity. Further, in-vitro prevention study of BIC NPs vs BIC solution was assessed against HIV-1 NLX and HIV-1 ADA on TZM-bl cell line and PBMCs, respectively. BIC nanoencapsulation demonstrated elevated cellular cytotoxicity concentration (CC 50 : 2.25 μM (BIC solution) to 820.4 μM (BIC NPs)] and lowers HIV-1 inhibitory concentration [EC 50 : 0.604 μM (BIC solution) to 0.0038 μM (BIC NPs)) thereby improving selectivity index (SI) from 3.7 (BIC solution) to 215,789 (BIC NP) for TZM-bl cells. Comparable results in PBMCs were obtained where BIC NPs improved SI from 0.29 (BIC solution) to 523.33 (BIC NPs). This demonstrates long-acting BIC nano-formulation with sustained drug-release potency, improved BIC cytotoxicity and enhanced HIV-1 protection compared to BIC in solution.

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“…Drugs were included into the PLGA/PVA system and investigated for their long-acting potency detectable even after 14 days by a humanized mice model [121,122]. A similar approach was exploited for the incorporation of TAF and elvitegravir, an integrase inhibitor, during the fabrication of devices to be used during vaginal prevention [123,124]. The drug absorption following oral administration were also positively affected by the use of TAF/PGLA loaded NPs, as highlighted by a statistical model study [125].…”

Section: Nucleoside Reverse Transcriptase Inhibitors Nanosystemsmentioning

confidence: 99%

Reverse Transcriptase Inhibitors Nanosystems Designed for Drug Stability and Controlled Delivery

et al. 2019

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An in-depth analysis of nanotechnology applications for the improvement of solubility, distribution, bioavailability and stability of reverse transcriptase inhibitors is reported. Current clinically used nucleoside and non-nucleoside agents, included in combination therapies, were examined in the present survey, as drugs belonging to these classes are the major component of highly active antiretroviral treatments. The inclusion of such agents into supramolecular vesicular systems, such as liposomes, niosomes and lipid solid NPs, overcomes several drawbacks related to the action of these drugs, including drug instability and unfavorable pharmacokinetics. Overall results reported in the literature show that the performances of these drugs could be significantly improved by inclusion into nanosystems.

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Pharmacokinetic and Tissue Distribution Profile of Long Acting Tenofovir Alafenamide and Elvitegravir Loaded Nanoparticles in Humanized Mice Model

Cited by 31 publications

References 21 publications

Long-acting parenteral combination antiretroviral loaded nano-drug delivery system to treat chronic HIV-1 infection: A humanized mouse model study

Long-acting parenteral combination antiretroviral loaded nano-drug delivery system to treat chronic HIV-1 infection: A humanized mouse model study

A potential long-acting bictegravir loaded nano-drug delivery system for HIV-1 infection: A proof-of-concept study

Reverse Transcriptase Inhibitors Nanosystems Designed for Drug Stability and Controlled Delivery

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