Literature DB >> 8973584

Bile pigments as HIV-1 protease inhibitors and their effects on HIV-1 viral maturation and infectivity in vitro.

F McPhee1, P S Caldera, G W Bemis, A F McDonagh, I D Kuntz, C S Craik.   

Abstract

Using recently developed molecular-shape description algorithms, we searched the Available Chemical Directory for known compounds similar in shape to the potent HIV-1 protease inhibitor Merck L-700,417; 15 compounds most similar in shape to the inhibitor were selected for testing in vitro. Four of these inhibited the protease at 100 microM or less and the most active of the four were the naturally occurring pigments biliverdin and bilirubin. Biliverdin and bilirubin inhibited recombinant HIV-1 protease in vitro at pH 7.8 with K1 values of approx. 1 microM, and also inhibited HIV-2 and simian immunodeficiency virus proteases. The related pyrrolic pigments stercobilin, urobilin, biliverdin dimethyl ester and xanthobilirubic acid showed similar inhibitory activity at low micromolar concentrations. Biliverdin, bilirubin and xanthobilirubic acid did not inhibit viral polyprotein processing in cultured cells, but they reduced viral infectivity significantly. At 100 microM, xanthobilirubic acid affected viral assembly, resulting in a 50% decrease in the generation of infectious particles. In contrast, at the same concentrations biliverdin and bilirubin exerted little or no effect on viral assembly but blocked infection of HeLaT4 cells by 50%. These results suggest that bile pigments might be a new class of potential lead compounds for developing protease inhibitors and they raise the question of whether hyperbilirubinaemia can influence the course of HIV infection.

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Year:  1996        PMID: 8973584      PMCID: PMC1217983          DOI: 10.1042/bj3200681

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  40 in total

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Authors:  I D Kuntz
Journal:  Science       Date:  1992-08-21       Impact factor: 47.728

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Authors:  L M Babé; C S Craik
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4.  In vivo emergence of HIV-1 variants resistant to multiple protease inhibitors.

Authors:  J H Condra; W A Schleif; O M Blahy; L J Gabryelski; D J Graham; J C Quintero; A Rhodes; H L Robbins; E Roth; M Shivaprakash
Journal:  Nature       Date:  1995-04-06       Impact factor: 49.962

5.  Preparation and properties of crystalline biliverdin IX alpha. Simple methods for preparing isomerically homogeneous biliverdin and [14C[biliverdin by using 2,3-dichloro-5,6-dicyanobenzoquinone.

Authors:  A F McDonagh; L A Palma
Journal:  Biochem J       Date:  1980-08-01       Impact factor: 3.857

Review 6.  Inhibitors of HIV-1 protease.

Authors:  T D Meek
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7.  Structure of a non-peptide inhibitor complexed with HIV-1 protease. Developing a cycle of structure-based drug design.

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8.  Role of hyperbilirubinemia in the impairment of osteoblast proliferation associated with cholestatic jaundice.

Authors:  C H Janes; E R Dickson; R Okazaki; S Bonde; A F McDonagh; B L Riggs
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10.  In vitro anti-human immunodeficiency virus type 1 activity of biliverdin, a bile pigment.

Authors:  H Mori; T Otake; M Morimoto; N Ueba; N Kunita; T Nakagami; N Yamasaki; S Taji
Journal:  Jpn J Cancer Res       Date:  1991-07
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  17 in total

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5.  Biosynthetically Distinct Cytotoxic Polyketides from Setophoma terrestris.

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Review 6.  Gut microbial metabolites associated with HIV infection.

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7.  Mechanism of indinavir-induced hyperbilirubinemia.

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8.  Induction of Heme Oxygenase-1 Deficiency and Associated Glutamate-Mediated Neurotoxicity Is a Highly Conserved HIV Phenotype of Chronic Macrophage Infection That Is Resistant to Antiretroviral Therapy.

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Review 9.  Bilirubin as a metabolic hormone: the physiological relevance of low levels.

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10.  Metalloprotoporphyrin Inhibition of HCV NS3-4A Protease: Structure-Activity Relationships.

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