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An Antibody-Recruiting Small Molecule That Targets HIV gp120

机译:抗体招聘小分子靶向HIV的gp120

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摘要

HIV/AIDS is a global pandemic for which new treatment strategies are desperately needed. We have designed a novel small molecule with the potential to interfere with HIV survival through two mechanisms: (1) by recruiting antibodies to gp120-expressing virus particles and infected human cells, thus enhancing their uptake and destruction by the human immune, and (2) by binding the viral glycoprotein gp120, inhibiting its interaction with the human protein CD4, and preventing virus entry. Here we demonstrate that ARM-H is capable of simultaneously binding gp120, a component of the Env surface viral glycoprotein (found on the surface of both HIV and virus-infected cells) and anti-2,4-dinitrophenyl antibodies (already present in the human bloodstream). The ternary complex formed between antibody, ARM-H, and gp120 is immunologically active and leads to the complement-mediated destruction of Env-expressing cells. Furthermore, ARM-H prevents virus entry into human T-cells, and should therefore be capable of inhibiting virus replication through two mutually reinforcing mechanisms (inhibition of virus entry and antibody-mediated killing). These studies demonstrate the viable anti-HIV activity of antibody-recruiting small molecules, and have the potential to initiate novel paradigms in HIV treatment.

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