Evidence for persistence of the SHIV reservoir early after MHC haploidentical hematopoietic stem cell transplantation

MHC单倍体相合造血干细胞移植后早期SHIV病毒库持续存在的证据

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作者:Lucrezia Colonna,Christopher W Peterson,John B Schell,Judith M Carlson,Victor Tkachev,Melanie Brown,Alison Yu,Sowmya Reddy,Willi M Obenza,Veronica Nelson,Patricia S Polacino,Heather Mack,Shiu-Lok Hu,Katie Zeleski,Michelle Hoffman,Joe Olvera,Scott N Furlan,Hengqi Zheng,Agne Taraseviciute,Daniel J Hunt,Kayla Betz,Jennifer F Lane,Keith Vogel,Charlotte E Hotchkiss,Cassie Moats,Audrey Baldessari,Robert D Murnane,Christopher English,Cliff A Astley,Solomon Wangari,Brian Agricola,Joel Ahrens,Naoto Iwayama,Andrew May,Laurence Stensland,Meei-Li W Huang,Keith R Jerome,Hans-Peter Kiem ,Leslie S Kean

Abstract

Allogeneic transplantation (allo-HCT) has led to the cure of HIV in one individual, raising the question of whether transplantation can eradicate the HIV reservoir. To test this, we here present a model of allo-HCT in SHIV-infected, cART-suppressed nonhuman primates. We infect rhesus macaques with SHIV-1157ipd3N4, suppress them with cART, then transplant them using MHC-haploidentical allogeneic donors during continuous cART. Transplant results in ~100% myeloid donor chimerism, and up to 100% T-cell chimerism. Between 9 and 47 days post-transplant, terminal analysis shows that while cell-associated SHIV DNA levels are reduced in the blood and in lymphoid organs post-transplant, the SHIV reservoir persists in multiple organs, including the brain. Sorting of donor-vs.-recipient cells reveals that this reservoir resides in recipient cells. Moreover, tetramer analysis indicates a lack of virus-specific donor immunity post-transplant during continuous cART. These results suggest that early post-transplant, allo-HCT is insufficient for recipient reservoir eradication despite high-level donor chimerism and GVHD.

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