Universal Tre (uTre) recombinase specifically targets the majority of HIV-1 isolates

Current drugs against HIV can suppress the progression to AIDS but cannot clear the patient from the virus. Because of potential side effects of these drugs and the possible development of drug resistance, finding a cure for HIV infection remains a high priority of HIV/AIDS research. We recently gen...

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Autores principales: Karpinski, Janet, Chemnitz, Jan, Hauber, Ilona, Abi-Ghanem, Josephine, Paszkowski-Rogacz, Maciej, Surendranath, Vineeth, Chakrabort, Debojyoti, Hackmann, Karl, Schröck, Evelin, Teresa Pisabarro, María, Hauber, Joachim, Buchholz, Frank
Formato: Online Artículo Texto
Lenguaje:English
Publicado: International AIDS Society 2014
Materias:
Poster Sessions – Abstract P174
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4225392/
https://www.ncbi.nlm.nih.gov/pubmed/25397454
http://dx.doi.org/10.7448/IAS.17.4.19706
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author Karpinski, Janet
Chemnitz, Jan
Hauber, Ilona
Abi-Ghanem, Josephine
Paszkowski-Rogacz, Maciej
Surendranath, Vineeth
Chakrabort, Debojyoti
Hackmann, Karl
Schröck, Evelin
Teresa Pisabarro, María
Hauber, Joachim
Buchholz, Frank
author_facet Karpinski, Janet
Chemnitz, Jan
Hauber, Ilona
Abi-Ghanem, Josephine
Paszkowski-Rogacz, Maciej
Surendranath, Vineeth
Chakrabort, Debojyoti
Hackmann, Karl
Schröck, Evelin
Teresa Pisabarro, María
Hauber, Joachim
Buchholz, Frank
author_sort Karpinski, Janet
collection PubMed
description Current drugs against HIV can suppress the progression to AIDS but cannot clear the patient from the virus. Because of potential side effects of these drugs and the possible development of drug resistance, finding a cure for HIV infection remains a high priority of HIV/AIDS research. We recently generated a recombinase (termed Tre) tailored to efficiently eradicate the provirus from the host genome of HIV-1 infected cells by specifically targeting a sequence that is present in the long terminal repeats (LTRs) of the viral DNA [1]. In vivo analyses in HIV-infected humanized mice demonstrated highly significant antiviral effects of Tre recombinase [2]. However, the fact that Tre recognizes a particular HIV-1 subtype A strain may limit its broad therapeutic application. To advance our Tre-based strategy towards a universally efficient cure, we have engineered a new, universal recombinase (uTre) applicable to the majority of HIV-1 infections by the various virus strains and subtypes. We employed the search tool SeLOX [3] in order to find a well-conserved HIV-1 proviral sequence that could serve as target site for a universal Tre from sequences compiled in the Los Alamos HIV Sequence Database. We selected a candidate (termed loxLTRu) with a mean conservation rate of 94% throughout the major HIV-1 subtype groups A, B and C. We applied loxLTRu as substrate in our established substrate-linked protein evolution (SLiPE) process [4] and evolved the uTre recombinase in 142 evolution cycles. Highly specific enzymatic activity on loxLTRu is demonstrated for uTre in both Escherichia coli and human cells. Naturally occurring viral variants with single mutations within the loxLTRu sequence are also shown to be efficiently targeted by uTre, further increasing the range of applicability of the recombinase. Potential off-target sites in the human genome are not recombined by uTre. Furthermore, uTre expression in primary human T cells shows no obvious Tre-related cytopathic or genotoxic effects. Finally, uTre expressing mice show no undesired phenotypes during their normal lifespan. We have developed a broad-range HIV-1 LTR specific recombinase that has the potential to be effective against the vast majority of HIV-1 strains and to cure HIV-1 infected cells from the infection. These results strongly encouraged us in our confidence that a Tre recombinase-mediated HIV eradication strategy may become a valuable component of a future therapy for HIV-infected patients.
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spelling pubmed-42253922014-11-13 Universal Tre (uTre) recombinase specifically targets the majority of HIV-1 isolates Karpinski, Janet Chemnitz, Jan Hauber, Ilona Abi-Ghanem, Josephine Paszkowski-Rogacz, Maciej Surendranath, Vineeth Chakrabort, Debojyoti Hackmann, Karl Schröck, Evelin Teresa Pisabarro, María Hauber, Joachim Buchholz, Frank J Int AIDS Soc Poster Sessions – Abstract P174 Current drugs against HIV can suppress the progression to AIDS but cannot clear the patient from the virus. Because of potential side effects of these drugs and the possible development of drug resistance, finding a cure for HIV infection remains a high priority of HIV/AIDS research. We recently generated a recombinase (termed Tre) tailored to efficiently eradicate the provirus from the host genome of HIV-1 infected cells by specifically targeting a sequence that is present in the long terminal repeats (LTRs) of the viral DNA [1]. In vivo analyses in HIV-infected humanized mice demonstrated highly significant antiviral effects of Tre recombinase [2]. However, the fact that Tre recognizes a particular HIV-1 subtype A strain may limit its broad therapeutic application. To advance our Tre-based strategy towards a universally efficient cure, we have engineered a new, universal recombinase (uTre) applicable to the majority of HIV-1 infections by the various virus strains and subtypes. We employed the search tool SeLOX [3] in order to find a well-conserved HIV-1 proviral sequence that could serve as target site for a universal Tre from sequences compiled in the Los Alamos HIV Sequence Database. We selected a candidate (termed loxLTRu) with a mean conservation rate of 94% throughout the major HIV-1 subtype groups A, B and C. We applied loxLTRu as substrate in our established substrate-linked protein evolution (SLiPE) process [4] and evolved the uTre recombinase in 142 evolution cycles. Highly specific enzymatic activity on loxLTRu is demonstrated for uTre in both Escherichia coli and human cells. Naturally occurring viral variants with single mutations within the loxLTRu sequence are also shown to be efficiently targeted by uTre, further increasing the range of applicability of the recombinase. Potential off-target sites in the human genome are not recombined by uTre. Furthermore, uTre expression in primary human T cells shows no obvious Tre-related cytopathic or genotoxic effects. Finally, uTre expressing mice show no undesired phenotypes during their normal lifespan. We have developed a broad-range HIV-1 LTR specific recombinase that has the potential to be effective against the vast majority of HIV-1 strains and to cure HIV-1 infected cells from the infection. These results strongly encouraged us in our confidence that a Tre recombinase-mediated HIV eradication strategy may become a valuable component of a future therapy for HIV-infected patients. International AIDS Society 2014-11-02 /pmc/articles/PMC4225392/ /pubmed/25397454 http://dx.doi.org/10.7448/IAS.17.4.19706 Text en © 2014 Karpinski J et al; licensee International AIDS Society http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Poster Sessions – Abstract P174
Karpinski, Janet
Chemnitz, Jan
Hauber, Ilona
Abi-Ghanem, Josephine
Paszkowski-Rogacz, Maciej
Surendranath, Vineeth
Chakrabort, Debojyoti
Hackmann, Karl
Schröck, Evelin
Teresa Pisabarro, María
Hauber, Joachim
Buchholz, Frank
Universal Tre (uTre) recombinase specifically targets the majority of HIV-1 isolates
title Universal Tre (uTre) recombinase specifically targets the majority of HIV-1 isolates
title_full Universal Tre (uTre) recombinase specifically targets the majority of HIV-1 isolates
title_fullStr Universal Tre (uTre) recombinase specifically targets the majority of HIV-1 isolates
title_full_unstemmed Universal Tre (uTre) recombinase specifically targets the majority of HIV-1 isolates
title_short Universal Tre (uTre) recombinase specifically targets the majority of HIV-1 isolates
title_sort universal tre (utre) recombinase specifically targets the majority of hiv-1 isolates
topic Poster Sessions – Abstract P174
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4225392/
https://www.ncbi.nlm.nih.gov/pubmed/25397454
http://dx.doi.org/10.7448/IAS.17.4.19706
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