<i>In Vitro</i>
            Selection of Highly Darunavir-Resistant and Replication-Competent HIV-1 Variants by Using a Mixture of Clinical HIV-1 Isolates Resistant to Multiple Conventional Protease Inhibitors

Koh, Yasuhiro; Amano, Masayuki; Towata, Tomomi; Danish, Matthew; Leshchenko-Yashchuk, Sofiya; Das, Debananda; Nakayama, Maki; Tojo, Yasushi; Ghosh, Arun K.; Mitsuya, Hiroaki

doi:10.1128/jvi.00967-10

Cited by 86 publications

(191 citation statements)

References 26 publications

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“…Koh et al (47) isolated HIV-1 variants from a patient failing PI-containing regimens. These viruses contained 9 to 14 protease mutations associated with PI resistance.…”

Section: Hiv-1 Env Mutations Can Confer Pi Resistance Even In the Conmentioning

confidence: 99%

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Multi-step inhibition explains HIV-1 protease inhibitor pharmacodynamics and resistance

Rabi

Laird²,

Durand³

et al. 2013

J. Clin. Invest.

125

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HIV-1 protease inhibitors (PIs) are among the most effective antiretroviral drugs. They are characterized by highly cooperative dose-response curves that are not explained by current pharmacodynamic theory. An unresolved problem affecting the clinical use of PIs is that patients who fail PI-containing regimens often have virus that lacks protease mutations, in apparent violation of fundamental evolutionary theory. Here, we show that these unresolved issues can be explained through analysis of the effects of PIs on distinct steps in the viral life cycle. We found that PIs do not affect virion release from infected cells but block entry, reverse transcription, and post-reverse transcription steps. The overall dose-response curves could be reconstructed by combining the curves for each step using the Bliss independence principle, showing that independent inhibition of multiple distinct steps in the life cycle generates the highly cooperative dose-response curves that make these drugs uniquely effective. Approximately half of the inhibitory potential of PIs is manifest at the entry step, likely reflecting interactions between the uncleaved Gag and the cytoplasmic tail (CT) of the Env protein. Sequence changes in the CT alone, which are ignored in current clinical tests for PI resistance, conferred PI resistance, providing an explanation for PI failure without resistance.

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“…Koh et al (47) isolated HIV-1 variants from a patient failing PI-containing regimens. These viruses contained 9 to 14 protease mutations associated with PI resistance.…”

Section: Hiv-1 Env Mutations Can Confer Pi Resistance Even In the Conmentioning

confidence: 99%

“…These viruses contained 9 to 14 protease mutations associated with PI resistance. The viruses were then grown in the presence of DRV for 51 passages and additional mutations in the protease gene accumulated (47). We cloned the full-length env gene from passages 1 and 51 (E-1 and E-51).…”

Section: Hiv-1 Env Mutations Can Confer Pi Resistance Even In the Conmentioning

confidence: 99%

Multi-step inhibition explains HIV-1 protease inhibitor pharmacodynamics and resistance

Rabi

Laird²,

Durand³

et al. 2013

J. Clin. Invest.

125

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“…However, we recently selected a highly DRV-resistant strain of HIV-1 in vitro by using a mixture of multi-PI-resistant (but DRV-sensitive) clinical HIV-1 strains as a starting viral population (7). In an attempt to examine the genetic barrier of GRL008, it was further evaluated against one of the DRV-resistant HIV-1 variants, HIV DRV R P20 (7) and was found to be potent, with only a 2.6-fold increase in its EC 50 above that for HIV WT . Although TPV showed a similar 2.7-fold increase in its EC 50 against HIV DRV R P20 , the absolute EC 50 of GRL008 was 3.5-fold lower than that of TPV, suggesting that GRL008 is overall a better PI than TPV against HIV DRV R P20 .…”

Section: Discussionmentioning

confidence: 99%

“…1), the latest FDA-approved protease inhibitor (PI), which contains bis-tetrahydrofuranyl urethane (bis-THF) as the P2 moiety, has been shown to have a high genetic barrier (5,6), a feature of a drug or regimen that delays or prevents the occurrence of genetic evolution of HIV-1 to acquire drug resistance-associated mutations, allowing the virus to overcome the antiretroviral activity of the very drug or regimen and to become capable of propagating despite treatment with the very drug or regimen. However, HIV-1 also ultimately develops high levels of resistance to DRV both in vitro and in vivo (7,8). In order to suppress the propagation of such PI-resistant HIV-1 protease variants, the development of novel PIs with greater antiviral activities and higher genetic barriers is urgently needed.…”

Section: H Uman Immunodeficiency Virus Type 1 (Hiv-1) Protease (Pr)mentioning

confidence: 99%

“…1) was evaluated against an MDR clinical isolate of HIV-1 (HIV A02 ) (10, 11) that contained eight amino acid substitutions, L10I, K45R, I54V, L63P, A71V, V82T, L90M, and I93L, in its protease (PR A02 ). The antiviral activity of GRL008 was also evaluated against HIV-2 ROD and an HIV-1 variant selected with DRV over 20 passages (HIV DRV R P20 ) (7). In addition, GRL008, DRV, ritonavir (RTV), and tipranavir (TPV) were individually cocrystallized with PR A02 , and a structure-function evaluation of each agent was performed.…”

Section: H Uman Immunodeficiency Virus Type 1 (Hiv-1) Protease (Pr)mentioning

confidence: 99%

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A Conserved Hydrogen-Bonding Network of P2 bis -Tetrahydrofuran-Containing HIV-1 Protease Inhibitors (PIs) with a Protease Active-Site Amino Acid Backbone Aids in Their Activity against PI-Resistant HIV

Yedidi

Garimella

Aoki

et al. 2014

Antimicrob Agents Chemother

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Verstärkung der Bindung an das Proteinrückgrat – ein fruchtbares Konzept gegen die Arzneimittelresistenz von HIV

et al. 2012

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Die Entstehung von Arzneimittelresistenzen ist eines der grundlegenden Probleme der Medizin. Dass sich bei HIV/AIDS so schnell resistente HIV‐1‐Varianten einstellen, ist ein großes Hindernis für die modernen Therapien. Wichtige Zielmoleküle der derzeitigen antiretroviralen Therapien sind Inhibitoren der HIV‐1‐Protease. Das Virus entwickelt Resistenzen, wenn Mutationen die Inhibitorbindung des Enzyms verändern und somit die Effizienz mindern. Um diese Resistenzbildung zu vermeiden, haben wir Inhibitoren erforscht, die am aktiven Zentrum der Protease Wasserstoffbrücken zum Proteinrückgrat bilden. Weil sich die Geometrie am katalytischen Zentrum ohne Funktionsverlust nicht ändern kann, schränken solche Wechselwirkungen die Möglichkeiten der Protease zur Resistenzbildung erheblich ein. Hier diskutieren wir das enzymatische Strukturprinzip, auf dem unser Konzept der Rückgratbindung beruht. Besonderes Augenmerk richten wir auf die Anwendung des Konzepts in unseren jüngeren Arbeiten zu antiviralen Inhibitoren der HIV‐1‐Protease.

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In Vitro Selection of Highly Darunavir-Resistant and Replication-Competent HIV-1 Variants by Using a Mixture of Clinical HIV-1 Isolates Resistant to Multiple Conventional Protease Inhibitors

Cited by 86 publications

References 26 publications

Multi-step inhibition explains HIV-1 protease inhibitor pharmacodynamics and resistance

Multi-step inhibition explains HIV-1 protease inhibitor pharmacodynamics and resistance

A Conserved Hydrogen-Bonding Network of P2 bis -Tetrahydrofuran-Containing HIV-1 Protease Inhibitors (PIs) with a Protease Active-Site Amino Acid Backbone Aids in Their Activity against PI-Resistant HIV

Verstärkung der Bindung an das Proteinrückgrat – ein fruchtbares Konzept gegen die Arzneimittelresistenz von HIV

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