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Dive into the research topics where Martin Robitaille is active.

Publication


Featured researches published by Martin Robitaille.


Journal of Biological Chemistry | 2008

Albumin-conjugated C34 Peptide HIV-1 Fusion Inhibitor EQUIPOTENT TO C34 AND T-20 IN VITRO WITH SUSTAINED ACTIVITY IN SCID-HU THY/LIV MICE

Cheryl A. Stoddart; Geneviève Nault; Sofiya A. Galkina; Karen Thibaudeau; Peter Bakis; Nathalie Bousquet-Gagnon; Martin Robitaille; Maryanne Bellomo; Véronique Paradis; Patricia Liscourt; Alexandra Lobach; Marie-Ève Rivard; Roger G. Ptak; Marie K. Mankowski; Dominique P. Bridon; Omar Quraishi

Entry inhibitors of human immunodeficiency virus, type 1 (HIV-1) have been the focus of much recent research. C34, a potent fusion inhibitor derived from the HR2 region of gp41, was engineered into a 1:1 human serum albumin conjugate through stable covalent attachment of a maleimido-C34 analog onto cysteine 34 of albumin. This bioconjugate, PC-1505, was designed to require less frequent dosing and less peptide than T-20 and was assessed for its antifusogenic activity both in vitro and in vivo in the SCID-hu Thy/Liv mouse model. PC-1505 was essentially equipotent to the original C34 peptide and to T-20 in vitro. In HIV-1-infected SCID-hu Thy/Liv mice, T-20 lost activity with infrequent dosing, whereas the antiviral potency of PC-1505 was sustained, and PC-1505 was active against T-20-resistant (“DIV”) virus with a G36D substitution in gp41. The in vivo results are the direct result of a significantly improved pharmacokinetic profile for the C34 peptide following albumin conjugation. Contrary to previous reports that the gp41 NHR trimer is poorly accessible to C34 fused to protein cargoes of increasing size (Hamburger, A. E., Kim, S., Welch, B. D., and Kay, M. S. (2005) J. Biol. Chem. 280, 12567–12572), these results are the first demonstration of the capacity for a large, endogenous serum protein to gain unobstructed access to the transient gp41 intermediates that exist during the HIV fusion process, and it supports further development of albumin conjugation as a promising approach to inhibit HIV-1 entry.


Bioorganic & Medicinal Chemistry Letters | 2003

Synthesis and In Vitro Analysis of Atrial Natriuretic Peptide-Albumin Conjugates

Roger Leger; Martin Robitaille; Omar Quraishi; Elizabeth Denholm; Corinne Benquet; Julie Carette; Pieter van Wyk; Isabelle Pellerin; Nathalie Bousquet-Gagnon; Jean-Paul Castaigne; Dominique P. Bridon

Atrial natriuretic peptide (ANP) is a clinically useful anti-hypertensive hormone. Maleimide derivatives of ANP have been synthesized and conjugated to cysteine-34 of human serum albumin. The conjugates were analyzed to assess their stability, receptor binding affinity and ability to stimulate guanylyl-cyclase activity in rat lung fibroblasts.


Journal of Biological Chemistry | 2007

A covalent inhibitor targeting an intermediate conformation of the fusogenic subunit of the HIV-1 envelope complex

Amy Jacobs; Omar Quraishi; Xicai Huang; Nathalie Bousquet-Gagnon; Geneviève Nault; Nicholas Francella; W. Gregory Alvord; Nga Pham; Chantal Soucy; Martin Robitaille; Dominique P. Bridon; Robert Blumenthal

Peptide inhibitors corresponding to sequences in the six helix bundle structure of the fusogenic portion (gp41) of the HIV envelope glycoprotein have been successfully implemented in preventing HIV entry. These peptides bind to regions in HIV gp41 transiently exposed during the fusion reaction. In an effort to improve upon these entry inhibitors, we have successfully designed and tested peptide analogs composed of chemical spacers and reactive moieties positioned strategically to facilitate covalent attachment. Using a temperature-arrested state prime wash in vitro assay we show evidence for the trapping of a pre-six helix bundle fusion intermediate by a covalent reaction with the specific anti-HIV-1 peptide. This is the first demonstration of the trapping of an intermediate conformation of a viral envelope glycoprotein during the fusion process that occurs in live cells. The permanent specific attachment of the covalent inhibitor is projected to improve the pharmacokinetics of administration in vivo and thereby improve the long-term sustainability of peptide entry inhibitor therapy and help to expand its applicability beyond salvage therapy.


Diabetes | 2003

Development and Characterization of a Glucagon-Like Peptide 1-Albumin Conjugate: The Ability to Activate the Glucagon-Like Peptide 1 Receptor In Vivo

Jung-Guk Kim; Laurie L. Baggio; Dominique P. Bridon; Jean-Paul Castaigne; Martin Robitaille; Lucie Jetté; Corinne Benquet; Daniel J. Drucker


Archive | 2000

Pulmonary delivery for bioconjugation

Alan M. Ezrin; Angelica Fleser; Martin Robitaille; Peter G. Milner; Dominique P. Bridon


Archive | 2005

Anti-obesity agents

Dominique P. Bridon; Roger Leger; Xicai Huang; Karen Thibaudeau; Martin Robitaille; Peter G. Milner


Bioorganic & Medicinal Chemistry Letters | 2004

Identification of CJC-1131-albumin bioconjugate as a stable and bioactive GLP-1(7–36) analog

Roger Leger; Karen Thibaudeau; Martin Robitaille; Omar Quraishi; Pieter van Wyk; Nathalie Bousquet-Gagnon; Julie Carette; Jean-Paul Castaigne; Dominique P. Bridon


Archive | 2000

Long lasting fusion peptide inhibitors for hiv infection

John W. Erickson; Dominique P. Bridon; Martin Robitaille; Grant A. Krafft; Dong Xie; Elena Afonina; Jun Liang; Sandra DeMeyer


Archive | 2003

Long lasting natriuretic peptide derivatives

Peter Bakis; Dominique P. Bridon; Julie Carette; Roger Leger; Martin Robitaille


Archive | 2000

Bioconjugation in vivo to pulmonary or blood components

Alan M. Ezrin; Angelica Fleser; Martin Robitaille; Peter G. Milner; Dominique P. Bridon

Collaboration


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Roger Leger

Université de Montréal

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Dong Xie

Science Applications International Corporation

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Elena Afonina

Science Applications International Corporation

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Amy Jacobs

University of Illinois at Chicago

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Marie K. Mankowski

Southern Research Institute

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