Chimeric antigen receptor (CAR)-T cell therapy has transformed the treatment of B-cell malignancies, but its success in acute myeloid leukemia (AML) remains limited. Durable responses depend on the formation of long-lived memory T cells, whereas T cell exhaustion contributes to non-response and relapse. In patients with AML who achieved remission after cord blood transplantation, we here first observe enrichment of memory T cells with high expression of the chemokine receptor CXCR4. Next, we show that engineering CAR-T cells to co-express CXCR4 enhances their persistence and anti-leukemic activity in patient-derived xenograft models. Using single-cell profiling and metabolic analysis, we find that CXCR4 promotes memory-associated transcriptional programs, reduces exhaustion, and supports oxidative metabolism. These effects are observed with CAR-T cells targeting CD25 or CD96 as AML-associated targets. Our results indicate that CXCR4 strengthens CAR-T cell memory and durability, offering a strategy to improve immunotherapy outcomes in AML and beyond.
CXCR4 induces memory formation over exhaustion in CAR-T cells to achieve durable leukemia targeting.
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作者:Itoh-Nakadai Ari, Liang Minggao, Shindo Michiho, Bibi Chen, Tomizawa-Murasawa Mariko, Fujiki Saera, Kaneko Akiko, Kanamaru Emi, Hashimoto Mari, Kajita Hiroshi, Ando Yoshinari, Kojima Miki, Moody Jonathan, Iwasaki Makoto, Takagi Shinsuke, Nakagawa Ryo, Agrawal Saumya, Amitani-Iijima Hanae, Sato Kaori, Sorimachi Yuriko, Suzuki Nahoko, Fukami Takehiro, Hanada Kazuharu, Morita Satoshi, Katsura Kazushige, Matsumoto Takehisa, Kobayashi Maiko, Kato Masahiko, Negishi Yasuyuki, Shirouzu Mikako, Najima Yuho, Takubo Keiyo, Hon Chung Chau, Uchida Naoyuki, Taniguchi Shuichi, Momozawa Yukihide, Carninci Piero, Shultz Leonard D, Saito Yoriko, de Hoon Michiel, Shin Jay W, Ishikawa Fumihiko
| 期刊: | Nature Communications | 影响因子: | 15.700 |
| 时间: | 2026 | 起止号: | 2026 Jan 26; 17(1):101 |
| doi: | 10.1038/s41467-025-67745-x | ||
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