Pitt Shield

CCR5-ligand decorated rilpivirine lipid-based nanoparticles for sustained antiretroviral responses.

Authors: Patel M, Panja S, Zaman LA, Yeapuri P, Bhattarai S, Gorantla S, Chang L, Heredia A, Walczak P, Hanson B, Cohen SM, Kevadiya BD, Gendelman HE

Antiretroviral therapy (ART) improves the quality of life for those living with the human immunodeficiency virus type one (HIV-1). However, poor compliance reduces ART effectiveness and leads to immune compromise, viral mutations, and disease co-morbidities. Here we develop a drug formulation in which a lipid-based nanoparticle (LBNP) carrying rilpivirine (RPV) is decorated with the C-C chemokine receptor type 5 (CCR5) targeting peptide. This facilitates extended drug persistence within myeloid cells. Particle delivery to viral reservoirs is tracked by positron emission tomography. The CCR5-mediated LBNP cell uptake and retention reduce HIV-1 replication in human monocyte-derived macrophages and infected humanized mice (hu mice). Focused ultrasound with microbubbles mediated blood brain barrier (BBB) disruption allows the CCR5-targeted LBNP to penetrate the BBB and reach brain myeloid cells. These findings offer a role for CCR5-targeted therapeutics in antiretroviral delivery to optimize HIV suppression.

Introduction

Purpose Drug delivery with BBB opening
Study Objective To develop and evaluate CCR5-targeted lipid-based rilpivirine nanoparticles that deliver antiretroviral drug to myeloid HIV reservoirs, including across the blood–brain barrier, to improve viral suppression.
Animal model / Human subject mouse, NSG, 20 weeks, not specified
Disease model HIV-1 infection (HIV/AIDS)
Targeted brain region(s) Brain
Cargo name and characteristics drug
Route of administration intravenous

Outcomes and Safety

Summary of Outcomes FUS-mediated BBB opening enabled delivery of CCR5-targeted rilpivirine nanoparticles to brain reservoirs and enhanced HIV suppression.
Duration of biological effect 25 days
Safety-related matter No adverse effects reported.

Brain Region

Ultrasound Parameters

Ultrasound instrument focused ultrasound transducer
FUS Frequency not reported
FUS Intensity not reported
FUS Pressure not reported
FUS Mode not reported
Pulse duration not reported
Duration of a single FUS session not reported
Treatment frequency single

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