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• W4385374803 abstract "ABSTRACT Background Appropriate interactions between antiretroviral therapies (ART) and drug transporters and metabolizing enzymes at the blood brain barrier (BBB) are critical to ensure adequate dosing of the brain to achieve HIV suppression. These proteins are modulated by demographic and lifestyle factors, including substance use. While understudied, illicit substances share drug transport and metabolism pathways with ART, increasing the potential for adverse drug:drug interactions. This is particularly important when considering the brain as it is relatively undertreated compared to peripheral organs and is vulnerable to substance use-mediated damage. Methods We used an in vitro model of the human BBB to determine the extravasation of three first-line ART drugs, emtricitabine (FTC), tenofovir (TFV), and dolutegravir (DTG), in the presence and absence of cocaine, which served as our illicit substance model. The impact of cocaine on BBB integrity and permeability, drug transporters, metabolizing enzymes, and their master transcriptional regulators were evaluated to determine the mechanisms by which substance use impacted ART central nervous system (CNS) availability. Results We determined that cocaine had a selective impact on ART extravasation, where it increased FTC’s ability to cross the BBB while decreasing TFV. DTG concentrations that passed the BBB were below quantifiable limits. Interestingly, the potent neuroinflammatory modulator, lipopolysaccharide, had no effect on ART transport, suggesting a specificity for cocaine. Unexpectedly, cocaine did not breach the BBB, as permeability to albumin and tight junction proteins and adhesion molecules remained unchanged. Rather, cocaine selectively decreased the pregnane-x receptor (PXR), but not constitutive androstane receptor (CAR). Consequently, drug transporter expression and activity decreased in endothelial cells of the BBB, including p-glycoprotein (P-gp), breast cancer resistance protein (BCRP), and multidrug resistance-associated protein 4 (MRP4). Further, cytochrome P450 3A4 (CYP3A4) enzymatic activity increased following cocaine treatment that coincided with decreased expression. Finally, cocaine modulated adenylate kinases are required to facilitate biotransformation of ART prodrugs to their phosphorylated, pharmacologically active counterparts. Conclusion Our findings indicate that additional considerations are needed in CNS HIV treatment strategies for people who use cocaine, as it may limit ART efficacy through regulation of drug transport and metabolizing pathways at the BBB." @default.
• W4385374803 created "2023-07-29" @default.
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• W4385374803 date "2023-07-29" @default.
• W4385374803 modified "2023-10-18" @default.
• W4385374803 title "Cocaine Regulates Antiretroviral Therapy CNS Access Through Pregnane-X Receptor-Mediated Drug Transporter and Metabolizing Enzyme Modulation at the Blood Brain Barrier" @default.
• W4385374803 cites W1239700790 @default.
• W4385374803 cites W1530364137 @default.
• W4385374803 cites W1575158876 @default.
• W4385374803 cites W1813855462 @default.
• W4385374803 cites W1831804007 @default.
• W4385374803 cites W1926912509 @default.
• W4385374803 cites W1968328048 @default.
• W4385374803 cites W1970489083 @default.
• W4385374803 cites W1979279465 @default.
• W4385374803 cites W1979607966 @default.
• W4385374803 cites W1986909190 @default.
• W4385374803 cites W1988971259 @default.
• W4385374803 cites W1990985572 @default.
• W4385374803 cites W1993881090 @default.
• W4385374803 cites W1996719014 @default.
• W4385374803 cites W1997190824 @default.
• W4385374803 cites W2000904449 @default.
• W4385374803 cites W2001453713 @default.
• W4385374803 cites W2001592123 @default.
• W4385374803 cites W2012700090 @default.
• W4385374803 cites W2012842635 @default.
• W4385374803 cites W2013110804 @default.
• W4385374803 cites W2015379298 @default.
• W4385374803 cites W2015896053 @default.
• W4385374803 cites W2017276225 @default.
• W4385374803 cites W2019647316 @default.
• W4385374803 cites W2020283319 @default.
• W4385374803 cites W2020610488 @default.
• W4385374803 cites W2021275669 @default.
• W4385374803 cites W2021444852 @default.
• W4385374803 cites W2023756943 @default.
• W4385374803 cites W2024028804 @default.
• W4385374803 cites W2029510824 @default.
• W4385374803 cites W2035837038 @default.
• W4385374803 cites W2043684815 @default.
• W4385374803 cites W2044911368 @default.
• W4385374803 cites W2048417224 @default.
• W4385374803 cites W2049733169 @default.
• W4385374803 cites W2050207944 @default.
• W4385374803 cites W2053186448 @default.
• W4385374803 cites W2056813461 @default.
• W4385374803 cites W2061843430 @default.
• W4385374803 cites W2062903449 @default.
• W4385374803 cites W2064478592 @default.
• W4385374803 cites W2065170135 @default.
• W4385374803 cites W2066349153 @default.
• W4385374803 cites W2070796637 @default.
• W4385374803 cites W2072667226 @default.
• W4385374803 cites W2073077090 @default.
• W4385374803 cites W2076161782 @default.
• W4385374803 cites W2077331899 @default.
• W4385374803 cites W2078068647 @default.
• W4385374803 cites W2079048674 @default.
• W4385374803 cites W2083172100 @default.
• W4385374803 cites W2088266524 @default.
• W4385374803 cites W2090458882 @default.
• W4385374803 cites W2092905779 @default.
• W4385374803 cites W2093044657 @default.
• W4385374803 cites W2093726594 @default.
• W4385374803 cites W2095217951 @default.
• W4385374803 cites W2097051924 @default.
• W4385374803 cites W2097113013 @default.
• W4385374803 cites W2097300084 @default.
• W4385374803 cites W2099500855 @default.
• W4385374803 cites W2101099825 @default.
• W4385374803 cites W2101949400 @default.
• W4385374803 cites W2109062146 @default.
• W4385374803 cites W2111596760 @default.
• W4385374803 cites W2117802425 @default.
• W4385374803 cites W2118335987 @default.
• W4385374803 cites W2130193551 @default.
• W4385374803 cites W2131731344 @default.
• W4385374803 cites W2134340301 @default.
• W4385374803 cites W2134388482 @default.
• W4385374803 cites W2138204804 @default.
• W4385374803 cites W2140135951 @default.
• W4385374803 cites W2147612239 @default.
• W4385374803 cites W2147968873 @default.
• W4385374803 cites W2148535109 @default.
• W4385374803 cites W2149385083 @default.
• W4385374803 cites W2151219710 @default.
• W4385374803 cites W2151945046 @default.
• W4385374803 cites W2152983548 @default.
• W4385374803 cites W2156015902 @default.
• W4385374803 cites W2164706038 @default.
• W4385374803 cites W2169205574 @default.

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