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Toward the development of a single-round infection assay based on EGFP reporting for anti-HIV-1 drug discovery.


ABSTRACT: BACKGROUND:The rapid increase of HIV-1 strains resistant to current antiretroviral drugs is a challenge for successful AIDS therapy. This necessitates the development of novel drugs, and to this end, availability of screening systems for in vitro drug discovery is a priority. Herein, we report the modification of a previously developed system for increased sensitivity, ease of use, and cost-efficiency, based on the application of the EGFP marker. METHODS:A PCR-amplified gfp gene (gfp) was cloned into pmzNL4-3, the plasmid already designed to produce single-cycle replicable virions, in frame with the reverse-transcriptase gene to construct the pmzNL4-3/GFP plasmid. GFP-mzNL4-3 pseudo-typed virions, as the first progeny viruses, were recovered from the culture supernatant of HEK293T cells co-transfected with pmzNL4-3/GFP and the helper plasmids pSPAX2 and pMD2G, which respectively encode HIV-1 Gag-Pol and vesicular stomatitis virus glycoprotein. Single-cycle replication and virion production were assessed by syncytia formation, p24 antigen assays, and electron and fluorescence microscopy. RESULTS:The incorporation of EGFP into the viral particles allowed their quantification by fluorometry, flow-cytometry, and fluorescence microscopy; however, this modification did not affect the single-round infectivity or production rate of the GFP fluorescence-emitting virions. CONCLUSIONS:Our results certify the development of a rapid, inexpensive, and safe GFP-reporting single-cycle replicable system for anti-HIV drug discovery. Further experiments are needed to measure the validity and robustness of the assay.

SUBMITTER: Soezi M 

PROVIDER: S-EPMC4757091 | biostudies-literature | 2015 Oct

REPOSITORIES: biostudies-literature

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Toward the development of a single-round infection assay based on EGFP reporting for anti-HIV-1 drug discovery.

Soezi Mahdieh M   Memarnejadian Arash A   Aminzadeh Saeed S   Zabihollahi Rezvan R   Sadat Seyed Mehdi SM   Amini Safieh S   Hekmat Soheila S   Aghasadeghi Mohammad Reza MR  

Reports of biochemistry & molecular biology 20151001 1


<h4>Background</h4>The rapid increase of HIV-1 strains resistant to current antiretroviral drugs is a challenge for successful AIDS therapy. This necessitates the development of novel drugs, and to this end, availability of screening systems for in vitro drug discovery is a priority. Herein, we report the modification of a previously developed system for increased sensitivity, ease of use, and cost-efficiency, based on the application of the EGFP marker.<h4>Methods</h4>A PCR-amplified gfp gene (  ...[more]

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