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NK cell recovery after haploidentical HSCT with posttransplant cyclophosphamide: Dynamics and clinical implications

Authors :
Maria Teresa Lupo Stanghellini
Raffaella Greco
Sofia Berglund
Leo Luznik
Francesca Lorentino
Giacomo Oliveira
Fabio Giglio
Andrea Assanelli
Mara Morelli
Valentina Gambacorta
Simona Piemontese
Jacopo Peccatori
Antonio Russo
Luca Vago
Nicoletta Cieri
Fabio Ciceri
Chiara Bonini
Cristina Toffalori
Laura Zito
Russo, Antonio
Oliveira, Giacomo
Berglund, Sofia
Greco, Raffaella
Gambacorta, Valentina
Cieri, Nicoletta
Toffalori, Cristina
Zito, Laura
Lorentino, Francesca
Piemontese, Simona
Morelli, Mara
Giglio, Fabio
Assanelli, Andrea
Stanghellini, Maria Teresa Lupo
Bonini, Chiara
Peccatori, Jacopo
Ciceri, Fabio
Luznik, Leo
Vago, Luca
Russo, A
Oliveira, G
Berglund, S
Greco, R
Gambacorta, V
Cieri, N
Toffalori, C
Zito, L
Lorentino, F
Piemontese, S
Morelli, M
Giglio, F
Assanelli, A
Stanghellini, M
Bonini, C
Peccatori, J
Ciceri, F
Luznik, L
Vago, L
Publication Year :
2018
Publisher :
American Society of Hematology, 2018.

Abstract

The use of posttransplant cyclophosphamide (PT-Cy) as graft-versus-host disease (GVHD) prophylaxis has revolutionized haploidentical hematopoietic stem cell transplantation (HSCT), allowing safe infusion of unmanipulated T cell-replete grafts. PT-Cy selectively eliminates proliferating alloreactive T cells, but whether and how it affects natural killer (NK) cells and their alloreactivity is largely unknown. Here we characterized NK cell dynamics in 17 patients who received unmanipulated haploidentical grafts, containing high numbers of mature NK cells, according to PT-Cy-based protocols in 2 independent centers. In both series, we documented robust proliferation of donor-derived NK cells immediately after HSCT. After infusion of Cy, a marked reduction of proliferating NK cells was evident, suggesting selective purging of dividing cells. Supporting this hypothesis, proliferating NK cells did not express aldehyde dehydrogenase and were killed by Cy in vitro. After ablation of mature NK cells, starting from day 15 after HSCT and favored by the high levels of interleukin-15 present in patients' sera, immature NK cells (CD62L+NKG2A+KIR-) became highly prevalent, possibly directly stemming from infused hematopoietic stem cells. Importantly, also putatively alloreactive single KIR+ NK cells were eliminated by PT-Cy and were thus decreased in numbers and antileukemic potential at day 30 after HSCT. As a consequence, in an extended series of 99 haplo-HSCT with PT-Cy, we found no significant difference in progression-free survival between patients with or without predicted NK alloreactivity (42% vs 52% at 1 year, P = NS). Our data suggest that the majority of mature NK cells infused with unmanipulated grafts are lost upon PT-Cy administration, blunting NK cell alloreactivity in this transplantation setting.

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....93c14b6a7e21c8ebd452bbc7a57a9581