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Small-Molecule Inhibition of HIV pre-mRNA Splicing as a Novel Antiretroviral Therapy to Overcome Drug Resistance
Author(s) -
Nadia Bakkour,
YeaLih Lin,
Sophie Maire,
Lilia Ayadi,
Florence MahuteauBetzer,
Chi Hung Nguyen,
Clément Mettling,
Pierre Portalès,
David S. Grierson,
Benoı̂t Chabot,
Philippe Jeanteur,
Christiane Branlant,
Pierre Corbeau,
Jamal Tazi
Publication year - 2007
Publication title -
plos pathogens
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.719
H-Index - 206
eISSN - 1553-7374
pISSN - 1553-7366
DOI - 10.1371/journal.ppat.0030159
Subject(s) - rna splicing , reverse transcriptase , biology , drug resistance , viral replication , virology , multiple drug resistance , gene , rna , virus , genetics
The development of multidrug-resistant viruses compromises antiretroviral therapy efficacy and limits therapeutic options. Therefore, it is an ongoing task to identify new targets for antiretroviral therapy and to develop new drugs. Here, we show that an indole derivative (IDC16) that interferes with exonic splicing enhancer activity of the SR protein splicing factor SF2/ASF suppresses the production of key viral proteins, thereby compromising subsequent synthesis of full-length HIV-1 pre-mRNA and assembly of infectious particles. IDC16 inhibits replication of macrophage- and T cell-tropic laboratory strains, clinical isolates, and strains with high-level resistance to inhibitors of viral protease and reverse transcriptase. Importantly, drug treatment of primary blood cells did not alter splicing profiles of endogenous genes involved in cell cycle transition and apoptosis. Thus, human splicing factors represent novel and promising drug targets for the development of antiretroviral therapies, particularly for the inhibition of multidrug-resistant viruses.

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