R01DA064139
Project Grant
Overview
Grant Description
Use of focused ultrasound stimulated blood brain barrier opening for CNS HIV/SIV reservoir reduction - Abstract
The advent of combination anti-retroviral therapy (CART) has prolonged the lifespans of people living with HIV.
However, upon cessation of ART treatment the virus quickly rebounds.
One of the likely causes for this rebound is the rapid seeding and establishment of viral reservoirs in multiple tissue compartments including the central nervous system (CNS).
The CNS is a sanctuary site for HIV due to the presence of barriers such as the blood brain barrier (BBB) and choroid plexus.
These structures significantly limit the CNS delivery of ART drugs which prevents control of viral replication and the associated negative effects on cognition.
Therefore, novel strategies need to be developed for both treatment and viral reservoir clearance in the brain.
We recently optimized a novel technique called focused ultrasound induced blood brain barrier opening (FUSS-BBBO) to overcome BBB permeability constraints.
FUS-BBBO has been safely and successfully used to deliver anticancer chemotherapy drugs directly into brain tumors in human patients and target large brain regions in rodents and nonhuman primates for gene delivery.
FUS-BBBO uses low-intensity ultrasound with systemically administered microbubbles, which oscillate in blood vessels at the ultrasound focus, resulting in safe, localized, temporary (6-24 h), and reversible opening of the BBB.
FUS-BBBO has been successfully used to deliver proteins, small molecules, and viral vectors without inflicting detectable tissue damage in both rodents and nonhuman primates.
Therefore, in the present study, we will use FUS-BBBO to deliver long-acting CART (cabotegravir and islatravir) drugs in conjunction with an anti-inflammatory delta-9-tetrahydrocannabinol treatment to two specific areas of the brain (basal ganglia and hippocampus) known to be targeted by HIV/SIV for better control of viral replication and persistence.
In addition, we will use adeno-associated vector particles to deliver a gene therapeutic blocking SIV infection (anti-SIV glycosylphosphatidylinositol-anchored single chain variable fragments (scFvs)) to brain resident macrophages and microglia for durable suppression of viral replication in the brain following CART interruption.
These new technologies will be tested in the SIV-infected rhesus macaque model that shows consistent CNS infection and neuroinflammation under suppressive CART.
While both cabotegravir and islatravir have been independently demonstrated to reduce plasma viremia in the human and rhesus macaques, our studies will for the first time directly test the efficacy of these drugs administered using subdermal nanofluidic implants on HIV/SIV replication in brain resident perivascular macrophages and microglia.
The proposed studies will help establish the FUS-BBBO method to increase CART drug delivery to the brain for reduction of neuro-HIV/SIV infection and its adverse effects on brain function.
Finally, these studies will also help evaluate the safety and efficacy of FUS-BBBO delivery of long-acting CARTs and novel AAV-delivered anti-HIV/SIV inhibitors to the brain.
The advent of combination anti-retroviral therapy (CART) has prolonged the lifespans of people living with HIV.
However, upon cessation of ART treatment the virus quickly rebounds.
One of the likely causes for this rebound is the rapid seeding and establishment of viral reservoirs in multiple tissue compartments including the central nervous system (CNS).
The CNS is a sanctuary site for HIV due to the presence of barriers such as the blood brain barrier (BBB) and choroid plexus.
These structures significantly limit the CNS delivery of ART drugs which prevents control of viral replication and the associated negative effects on cognition.
Therefore, novel strategies need to be developed for both treatment and viral reservoir clearance in the brain.
We recently optimized a novel technique called focused ultrasound induced blood brain barrier opening (FUSS-BBBO) to overcome BBB permeability constraints.
FUS-BBBO has been safely and successfully used to deliver anticancer chemotherapy drugs directly into brain tumors in human patients and target large brain regions in rodents and nonhuman primates for gene delivery.
FUS-BBBO uses low-intensity ultrasound with systemically administered microbubbles, which oscillate in blood vessels at the ultrasound focus, resulting in safe, localized, temporary (6-24 h), and reversible opening of the BBB.
FUS-BBBO has been successfully used to deliver proteins, small molecules, and viral vectors without inflicting detectable tissue damage in both rodents and nonhuman primates.
Therefore, in the present study, we will use FUS-BBBO to deliver long-acting CART (cabotegravir and islatravir) drugs in conjunction with an anti-inflammatory delta-9-tetrahydrocannabinol treatment to two specific areas of the brain (basal ganglia and hippocampus) known to be targeted by HIV/SIV for better control of viral replication and persistence.
In addition, we will use adeno-associated vector particles to deliver a gene therapeutic blocking SIV infection (anti-SIV glycosylphosphatidylinositol-anchored single chain variable fragments (scFvs)) to brain resident macrophages and microglia for durable suppression of viral replication in the brain following CART interruption.
These new technologies will be tested in the SIV-infected rhesus macaque model that shows consistent CNS infection and neuroinflammation under suppressive CART.
While both cabotegravir and islatravir have been independently demonstrated to reduce plasma viremia in the human and rhesus macaques, our studies will for the first time directly test the efficacy of these drugs administered using subdermal nanofluidic implants on HIV/SIV replication in brain resident perivascular macrophages and microglia.
The proposed studies will help establish the FUS-BBBO method to increase CART drug delivery to the brain for reduction of neuro-HIV/SIV infection and its adverse effects on brain function.
Finally, these studies will also help evaluate the safety and efficacy of FUS-BBBO delivery of long-acting CARTs and novel AAV-delivered anti-HIV/SIV inhibitors to the brain.
Funding Goals
NOT APPLICABLE
Grant Program (CFDA)
Awarding / Funding Agency
Place of Performance
San Antonio,
Texas
782275302
United States
Geographic Scope
Single Zip Code
Analysis Notes
Amendment Since initial award the total obligations have increased 74% from $1,825,990 to $3,170,056.
Texas Biomedical Research Institute was awarded
Focused Ultrasound for CNS HIV Reservoir Reduction
Project Grant R01DA064139
worth $3,170,056
from National Institute on Drug Abuse in September 2025 with work to be completed primarily in San Antonio Texas United States.
The grant
has a duration of 4 years 8 months and
was awarded through assistance program 93.279 Drug Abuse and Addiction Research Programs.
The Project Grant was awarded through grant opportunity Advancing Technologies to Improve Delivery of Pharmacological, Gene Editing, and other Cargoes for HIV and SUD Mechanistic or Therapeutic Research (R01 Clinical Trial Optional).
Status
(Ongoing)
Last Modified 5/21/26
Period of Performance
9/1/25
Start Date
5/31/30
End Date
Funding Split
$3.2M
Federal Obligation
$0.0
Non-Federal Obligation
$3.2M
Total Obligated
Activity Timeline
Transaction History
Modifications to R01DA064139
Additional Detail
Award ID FAIN
R01DA064139
SAI Number
R01DA064139-3412593655
Award ID URI
SAI UNAVAILABLE
Awardee Classifications
Nonprofit With 501(c)(3) IRS Status (Other Than An Institution Of Higher Education)
Awarding Office
75N600 NIH National Insitute on Drug Abuse
Funding Office
75N600 NIH National Insitute on Drug Abuse
Awardee UEI
J4EYPCJDQ1H6
Awardee CAGE
02MD3
Performance District
TX-20
Senators
John Cornyn
Ted Cruz
Ted Cruz
Modified: 5/21/26