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. 2025 Apr;6(4):595-611.
doi: 10.1038/s43018-025-00934-1. Epub 2025 Mar 24.

CAR T or NK cells targeting mismatched HLA-DR molecules in acute myeloid leukemia after allogeneic hematopoietic stem cell transplant

Shunya Ikeda #  1 Kana Hasegawa #  1   2 Yosuke Kogue #  3   4 Takao Arimori  5 Ryuhei Kawamoto  6 Tansri Wibowo  7 Moto Yaga  7 Yuri Inada  6 Hirofumi Uehara  6 Miwa Matsubara  6 Mana Tachikawa  6 Makiko Suga  4 Shuhei Kida  4 Kumi Shibata  4 Kazuhito Tsutsumi  4 Kentaro Fukushima  4 Jiro Fujita  4 Tomoaki Ueda  4 Shinsuke Kusakabe  4 Akihisa Hino  4 Michiko Ichii  4 Asao Hirose  8 Hirohisa Nakamae  8 Masayuki Hino  8 Takafumi Nakao  9 Megumu Inoue  10 Kyoko Yoshihara  11 Satoshi Yoshihara  11 Shuji Ueda  12 Tetsuro Tachi  13 Hideki Kuroda  13 Koki Murakami  13 Noriyuki Kijima  13 Haruhiko Kishima  13 Eri Igashira  14 Mari Murakami  14 Tsuyoshi Takiuchi  15 Tadashi Kimura  15 Takashi Hiroshima  16 Toru Kimura  16 Yasushi Shintani  16 Chihaya Imai  17 Kosuke Yusa  18 Ryota Mori  19 Takayuki Ogino  19 Hidetoshi Eguchi  19 Kiyoshi Takeda  1   14   20   21 Yusuke Oji  6 Atsushi Kumanogoh  1   7   20   21 Junichi Takagi  5 Naoki Hosen  22   23   24   25
Affiliations

CAR T or NK cells targeting mismatched HLA-DR molecules in acute myeloid leukemia after allogeneic hematopoietic stem cell transplant

Shunya Ikeda et al. Nat Cancer. 2025 Apr.

Abstract

Acute myeloid leukemia (AML)-specific target antigens are difficult to identify. Here we demonstrate that HLA-DRB1 can serve as a leukemia-specific target of chimeric antigen receptor (CAR) T cells in patients with AML after allogeneic hematopoietic stem cell transplantation (allo-HCT). We identified KG2032 as a monoclonal antibody specifically bound to AML cells in about half of patients, but not to normal leukocytes other than B lymphocytes. KG2032 reacted with a subset of HLA-DRB1 molecules, specifically those in which the 86th amino acid was not aspartic acid. KG2032 reacted minimally with nonhematopoietic tissues. These results indicate that KG2032 reactivity is highly specific for AML cells in patients who carry KG2032-reactive HLA-DRB1 alleles and who received allo-HCT from a donor carrying KG2032-nonreactive HLA-DRB1 alleles. KG2032-derived CAR T or natural killer cells showed significant anti-leukemic activity in preclinical models in female mice, suggesting that they may cure patients with AML who are incurable with allo-HCT.

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Conflict of interest statement

Competing interests: N.H. has applied for a patent entitled ‘Antibody against acute myeloid leukemia’ (PCT/JP2023/042029) through the Osaka University Office for University–Industry Collaboration. The other authors declare no competing interests.

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