Your search keyword '"De La Cruz, Gabriela"' showing total 3 results

1. Heterogeneous antiretroviral drug distribution and HIV/SHIV detection in the gut of three species.

Author

Thompson CG, Rosen EP, Prince HMA, White N, Sykes C, de la Cruz G, Mathews M, Deleage C, Estes JD, Charlins P, Mulder LR, Kovarova M, Adamson L, Arora S, Dellon ES, Peery AF, Shaheen NJ, Gay C, Muddiman DC, Akkina R, Garcia JV, Luciw P, and Kashuba ADM

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Adolescent, Adult, Aged, Animals, CD3 Complex metabolism, Female, Gastrointestinal Tract drug effects, Gene Expression Regulation, Viral drug effects, HIV genetics, Humans, Macaca mulatta, Male, Mice, Middle Aged, RNA, Viral genetics, RNA, Viral metabolism, Simian Immunodeficiency Virus genetics, Species Specificity, T-Lymphocytes drug effects, Young Adult, Anti-Retroviral Agents pharmacology, Gastrointestinal Tract virology, HIV drug effects, Simian Immunodeficiency Virus drug effects

Abstract

HIV replication within tissues may increase in response to a reduced exposure to antiretroviral drugs. Traditional approaches to measuring drug concentrations in tissues are unable to characterize a heterogeneous drug distribution. Here, we used mass spectrometry imaging (MSI) to visualize the distribution of six HIV antiretroviral drugs in gut tissue sections from three species (two strains of humanized mice, macaques, and humans). We measured drug concentrations in proximity to CD3 + T cells that are targeted by HIV, as well as expression of HIV or SHIV RNA and expression of the MDR1 drug efflux transporter in gut tissue from HIV-infected humanized mice, SHIV-infected macaques, and HIV-infected humans treated with combination antiretroviral drug therapy. Serial 10-μm sections of snap-frozen ileal and rectal tissue were analyzed by MSI for CD3 + T cells and MDR1 efflux transporter expression by immunofluorescence and immunohistochemistry, respectively. The tissue slices were analyzed for HIV/SHIV RNA expression by in situ hybridization and for antiretroviral drug concentrations by liquid chromatography-mass spectrometry. The gastrointestinal tissue distribution of the six drugs was heterogeneous. Fifty percent to 60% of CD3 + T cells did not colocalize with detectable drug concentrations in the gut tissue. In all three species, up to 90% of HIV/SHIV RNA was found to be expressed in gut tissue with no exposure to drug. These data suggest that there may be gut regions with little to no exposure to antiretroviral drugs, which may result in low-level HIV replication contributing to HIV persistence., (Copyright © 2019 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2019

2. Antiretroviral concentrations and surrogate measures of efficacy in the brain tissue and CSF of preclinical species.

Author

Srinivas, Nithya, Rosen, Elias P., Gilliland Jr, William M., Kovarova, Martina, Remling-Mulder, Leila, De La Cruz, Gabriela, White, Nicole, Adamson, Lourdes, Schauer, Amanda P., Sykes, Craig, Luciw, Paul, Garcia, J. Victor, Akkina, Ramesh, and Kashuba, Angela D. M.

Subjects

CEREBROSPINAL fluid, BRAIN, RHESUS monkeys, PROTEIN binding, TISSUES, AUTOPSY

Abstract

1. Antiretroviral concentrations in cerebrospinal fluid (CSF) are used as surrogate for brain tissue, although sparse data support this. We quantified antiretrovirals in brain tissue across preclinical models, compared them to CSF, and calculated 90% inhibitory quotients (IQ90) for nonhuman primate (NHP) brain tissue. Spatial distribution of efavirenz was performed by mass-spectrometry imaging (MSI). 2. HIV or RT-SHIV-infected and uninfected animals from two humanized mouse models (hemopoietic-stem cell/RAG2-, n = 36; bone marrow-liver-thymus/BLT, n =13) and an NHP model (rhesus macaque, n =18) were dosed with six antiretrovirals. Brain tissue, CSF (NHPs), and plasma were collected at necropsy. Drug concentrations were measured by LC-MS/MS. Rapid equilibrium dialysis determined protein binding in NHP brain. 3. Brain tissue penetration of most antiretrovirals were >10-fold lower (p < 0.02) in humanized mice than NHPs. NHP CSF concentrations were >13-fold lower (p <0.02) than brain tissue with poor agreement except for efavirenz (r = 0.91, p = 0.001). Despite 97% brain tissue protein binding, efavirenz achieved IQ90>1 in all animals and 2-fold greater white versus gray matter concentration. 4. Brain tissue penetration varied across animal models for all antiretrovirals except raltegravir, and extrapolating brain tissue concentrations between models should be avoided. With the exception of efavirenz, CSF is not a surrogate for brain tissue concentrations. [ABSTRACT FROM AUTHOR]

Published

2019

3. Long-acting injectable multipurpose prevention technology for prevention of HIV and unplanned pregnancy.

Author

Young, Isabella C., Pallerla, Aryani, Cottrell, Mackenzie L., Maturavongsadit, Panita, Prasher, Alka, Shrivastava, Roopali, De la Cruz, Gabriela, Montgomery, Stephanie A., Schauer, Amanda, Sykes, Craig, Kashuba, Angela D.M., and Benhabbour, S. Rahima

Subjects

*UNPLANNED pregnancy, *CONTRACEPTIVE drugs, *HIV, *MEDROXYPROGESTERONE, *CONTRACEPTIVES, *CONTRACEPTION, *LONG-acting reversible contraceptives

Abstract

Only condoms are proven to protect against both HIV and unplanned pregnancy, however, poor user acceptability and lack of partner cooperation impede effectiveness. We developed an injectable ultra-long-acting, biodegradable, and removable in-situ forming implant (ISFI) as multipurpose prevention technology (MPT). MPT ISFIs co-formulated an antiretroviral (dolutegravir (DTG)) or cabotegravir (CAB)), and a hormonal contraceptive (etonogestrel (ENG) or medroxyprogesterone acetate (MPA)). All formulations were well-tolerated in mice with no signs of chronic local or systemic inflammation. Plasma CAB and DTG concentrations were above 4 × PA-IC 90 for 90 days with zero-order and diffusion-controlled absorption, respectively, and no differences when co-formulated with either hormone. Plasma ENG and MPA concentrations were quantifiable for 90 days. Complete removal of CAB/MPA ISFIs resulted in MPA concentrations falling below the limit of quantification after 24 h post-removal, but incomplete CAB elimination from plasma. Collectively, we demonstrated the ability to co-formulate antiretrovirals with contraceptives in an ISFI that is well-tolerated with sustained plasma concentrations up to 90 days. [Display omitted] • Co-formulation of an antiretroviral (ARV) and contraceptive drug in a single injection. • All injectable formulations were safe and well-tolerated in BALB/c mice. • ARV concentration in plasma was above PK benchmark for HIV PrEP of 4× PA-IC 90 for 90 days. • First-in-line long-acting injectable multipurpose prevention technology. [ABSTRACT FROM AUTHOR]

Published

2023