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2 research outputs found

Potent and broad HIV-neutralizing antibodies in memory B cells and plasma

Author: Anasti K.
Bailer R.T.
Bonsignori M.
Bradley T.
Cohen M.S.
Gao F.
Georgiev I.S.
Georgiou G.
Haynes B.F.
Kamanga G.
Kelsoe G.
Kepler T.B.
Korber B.
Liao H.-X.
Louder M.K.
Lougheed C.S.
Lu X.
Marshall D.J.
Mascola J.R.
McDaniel J.R.
McKee K.
Montefiori D.C.
Moody M.A.
Morris L.
Munir Alam S.
Nicely N.I.
Nie X.
Ofek G.
O’Dell S.
Parks R.J.
Saunders K.O.
Schätzle S.
Seaman M.S.
Tomaras G.D.
Tumba N.L.
Wagh K.
Wiehe K.
Williams L.D.
Wu L.
Xia S.-M.
Yang G.
Publication venue: American Association for the Advancement of Science
Publication date: 01/01/2017
Field of study

Induction of broadly neutralizing antibodies (bnAbs) is a goal of HIV-1 vaccine development. Antibody 10E8, reactive with the distal portion of the membrane-proximal external region (MPER) of HIV-1 gp41, is broadly neutralizing. However, the ontogeny of distal MPER antibodies and the relationship of memory B cell to plasma bnAbs are poorly understood. HIV-1–specific memory B cell flow sorting and proteomic identification of anti-MPER plasma antibodies from an HIV-1–infected individual were used to isolate broadly neutralizing distal MPER bnAbs of the same B cell clonal lineage. Structural analysis demonstrated that antibodies from memory B cells and plasma recognized the envelope gp41 bnAb epitope in a distinct orientation compared with other distal MPER bnAbs. The unmutated common ancestor of this distal MPER bnAb was autoreactive, suggesting lineage immune tolerance control. Construction of chimeric antibodies of memory B cell and plasma antibodies yielded a bnAb that potently neutralized most HIV-1 strains

Carolina Digital Repository

Strain-Specific V3 and CD4 Binding Site Autologous HIV-1 Neutralizing Antibodies Select Neutralization-Resistant Viruses

Author: Alam S.M.
Amos J.D.
Bonsignori M.
Cohen M.S.
Ferrari G.
Finzi A.
Gao F.
Gorny M.K.
Grey Elin S.
Gurley T.C.
Hahn B.H.
Haynes B.F.
Hora B.
Hraber P.T.
Hwang K.-K.
Kamanga G.
Kapiga S.
Korber B.T.
Kumar A.
Liao H.-X.
Llyod K.E.
Lu X.
Marshall D.J.
Mascola J.R.
Montefiori D.C.
Moody M.A.
Morris L.
Parks R.
Sam N.E.
Shaw G.M.
Shen X.
Sodroski J.G.
Tomaras G.D.
Tumba N.L.
Vandergrift N.A.
Whitesides J.F.
Xia S.-M.
Zolla-Pazner S.
Publication venue: 'Elsevier BV'
Publication date: 01/01/2015
Field of study

The third variable (V3) loop and the CD4 binding site (CD4bs) of the HIV-1 envelope are frequently targeted by neutralizing antibodies (nAbs) in infected individuals. In chronic infection, HIV-1 escape mutants repopulate the plasma, and V3 and CD4bs nAbs emerge that can neutralize heterologous tier 1 easy-to-neutralize but not tier 2 difficult-to-neutralize HIV-1 isolates. However, neutralization sensitivity of autologous plasma viruses to this type of nAb response has not been studied. We describe the development and evolution in vivo of antibodies distinguished by their target specificity for V3 and CD4bs epitopes on autologous tier 2 viruses but not on heterologous tier 2 viruses. A surprisingly high fraction of autologous circulating viruses was sensitive to these antibodies. These findings demonstrate a role for V3 and CD4bs antibodies in constraining the native envelope trimer in vivo to a neutralization-resistant phenotype, explaining why HIV-1 transmission generally occurs by tier 2 neutralization-resistant viruses

Research Online @ ECU