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Abstract

The α₄β₇ is a lymphocyte homing receptor to the gut-associated lymphoid tissue (GALT). HIV-1 gp120 binds to α₄β₇ integrin through a mimetic tripeptide in V2 and ensures successful infection of GALT. In the present report, we investigated the presence of polymorphisms in the α₄β₇ cytoplasmic and α₄ N-terminal binding domains and their potential association with susceptibility to HIV infection or disease progression. Subjects displaying distinct categories of disease progression or transmission routes (HIV-positive adults, vertically infected infants, and seronegative subjects) had their ITGA4 and ITGB7 gene segments corresponding to virus binding sites and C-terminal domains PCR amplified and sequenced. An absolute conservation of the studied regions was observed in all patients and controls. Albeit polymorphisms in α₄β₇ may exist in other regions not tracked in this study, α₄β₇ activation and binding domains do not seem to be polymorphic and are not correlated with distinct patterns of HIV transmission or disease progression.

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Conservation of the α 4 β 7 Lymphocyte Homing Receptor in HIV-Infected Patients with Distinct Transmission Routes and Disease Progression Profiles

Abstract

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