A J Langlois
Duke University
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Featured researches published by A J Langlois.
Science | 1990
K Javaherian; A J Langlois; Gj LaRosa; At Profy; Dani P. Bolognesi; Wc Herlihy; Scott D. Putney; T J Matthews
The principal neutralizing determinant (PND) of human immunodeficiency virus (HIV)-1 resides within the V3 loop of the envelope protein. Antibodies elicited by peptides of this region were able to neutralize diverse isolates. Serum from one of three animals immunized with the human T cell lymphoma virus (HTLV)-IIIMN PND peptide, RP142, neutralized MN and the sequence-divergent HTLV-IIIB isolate. Serum from one of three animals immunized with a 13-amino acid IIIB PND peptide (RP337) also neutralized both of these isolates. Characterization of these sera revealed that the cross-neutralizing antibodies bound the amino acid sequence GlyProGlyArgAlaPhe (GPGRAF) that is present in both isolates. This sequence is frequently found in the PNDs analyzed in randomly selected HIV-1 isolates. Sera from two rabbits immunized with a peptide containing only the GPGRAF residues neutralized divergent isolates, including IIIB and MN.
The Lancet | 1988
KentJ. Weinhold; T J Matthews; PaulM. Ahearne; A J Langlois; H. Kim Lyerly; DouglasS. Tyler; KimoC. Stine; D T Durack; DaniP. Bolognesi
Forty-one patients seropositive for human immunodeficiency virus type 1 (HIV-1) were assessed for cell-mediated cytotoxicity (CMC) against autologous target cells bearing the major envelope glycoprotein of HIV-1, gp120. Effector lymphocytes from over 85% of seropositive patients showed CMC specific for gp120-coated targets, whereas seronegative individuals had no detectable CMC. As a group, symptomless individuals had the highest levels of CMC; patients with AIDS-related complex and AIDS showed progressively diminished reactivity. The gp120-specific CMC was mediated by a population of non-T-cell effectors phenotypically resembling NK/K cells. Cytolysis was not restricted by major histocompatibility complex determinants, as shown by killing of heterologous gp120-adsorbed targets and of HIV-1-infected cell-lines. Gp120-specific CMC was highly augmented in the presence of interleukin 2, so it may be possible to develop therapeutic strategies aimed at destruction of virus-producing cell reservoirs in infected individuals through stimulation of HIV-specific host CMC.
Science | 1990
Gj LaRosa; Jp Davide; Kent J. Weinhold; Ja Waterbury; At Profy; Ja Lewis; A J Langlois; Gr Dreesman; Rn Boswell; Shadduck Pp
Proceedings of the National Academy of Sciences of the United States of America | 1989
Kashi Javaherian; A J Langlois; C McDanal; K L Ross; L I Eckler; C L Jellis; At Profy; James R. Rusche; Dani P. Bolognesi; Scott D. Putney
Proceedings of the National Academy of Sciences of the United States of America | 1988
James R. Rusche; K Javaherian; C McDanal; J Petro; D L Lynn; R Grimaila; A J Langlois; Robert C. Gallo; L O Arthur; P J Fischinger
Proceedings of the National Academy of Sciences of the United States of America | 1988
Thomas J. Palker; M E Clark; A J Langlois; T J Matthews; Kent J. Weinhold; R R Randall; Dani P. Bolognesi; Barton F. Haynes
Science | 1986
Scott D. Putney; T J Matthews; Wg Robey; Dl Lynn; M Robert-Guroff; Wt Mueller; A J Langlois; J Ghrayeb; Stephen Robert Petteway; Kent J. Weinhold
Antimicrobial Agents and Chemotherapy | 1987
M H St Clair; C A Richards; Thomas Spector; Kent J. Weinhold; W H Miller; A J Langlois; P A Furman
Proceedings of the National Academy of Sciences of the United States of America | 1986
W G Robey; L O Arthur; T J Matthews; A J Langlois; T D Copeland; N W Lerche; S Oroszlan; Dani P. Bolognesi; Raymond V. Gilden; Peter J. Fischinger
Proceedings of the National Academy of Sciences of the United States of America | 1987
Herbert Kim Lyerly; T J Matthews; A J Langlois; Dani P. Bolognesi; Kent J. Weinhold
