结直肠癌中CD38（高）CD16（低）NK细胞的高比例可以中断免疫监视并促进肿瘤生长。

Cancer immunology, immunotherapy : CII Pub Date : 2025-07-12 DOI:10.1007/s00262-025-04044-w

Xueling Wang, Li Li, Xianqin Song, Kehua Fang, Xiaotian Chang

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摘要

CD38 + NK细胞已在许多疾病中被检测到。本研究探讨了CD38 + NK细胞在肿瘤免疫监视中的作用机制。流式细胞术检测发现，乳腺癌、结直肠癌（CRC）、食管癌、胃癌（GC）、肺癌（LG）、卵巢癌（OC）患者外周血中CD38 + NK细胞比例显著升高。转录组学和代谢组学揭示了CRC CD38 + NK细胞的特殊表达谱和代谢物丰度模式，特别是HSPA1（热休克70 kDa蛋白1A）降低和ADO（腺苷）水平升高。与健康人CD38 + NK细胞相比，CRC CD38 + NK细胞产生NAD +（烟酰胺腺嘌呤二核苷酸）、诱导凋亡和杀伤肿瘤细胞的能力较低，浸润肿瘤组织和诱导肿瘤细胞增殖的能力较高。CRC CD38 + NK细胞也产生较少的tnf - α和较多的IL-2、ADO和tgf - β。当用抗CD38抗体预处理CD38 + NK细胞时，得到相反的结果，ifn - γ的产生增加。移植小鼠结肠癌源性MC38细胞的野生型C57BL/6 J小鼠肿瘤生长明显加快，外周血Treg和CD38 + NK细胞水平升高，Th1细胞水平降低。此外，通过实时荧光定量PCR和Western blot分析，CRC CD38 + NK细胞中CD38、PD-1和NF-kB表达升高，CD16、Sirt1、Sirt6和HSPA1表达降低，表明NK细胞表达高CD38和低CD16。CRC、GC、LC和OC患者血液中CD38 + CD16- NK细胞比例较高。众所周知，高Tregs、tgf - β、PD-1和ADO水平以及低HSPA1、NAD +、tnf - α和ifn - γ水平有助于免疫肿瘤细胞的逃逸。我们的研究结果表明，肿瘤患者中CD38（高）CD16（低）NK细胞的高比例可以中断免疫监视并促进肿瘤生长。

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A high proportion of CD38 (high) CD16 (low) NK cells in colorectal cancer can interrupt immune surveillance and favor tumor growth.

CD38 + NK cells have been detected in many diseases. The present study investigated the mechanism of CD38 + NK cells in immune surveillance in tumors. Significant increases in the proportions of CD38 + NK cells were detected via flow cytometry in the peripheral blood of patients with breast cancer, colorectal cancer (CRC), esophageal cancer, gastric cancer (GC), lung cancer (LG) or ovarian cancer (OC). Transcriptomics and metabonomics revealed special expression profiles and metabolite abundance patterns in CRC CD38 + NK cells, especially decreased HSPA1 (heat shock 70 kDa protein 1A) and increased ADO (adenosine) levels. Compared with CD38 + NK cells from healthy individuals, CRC CD38 + NK cells presented lower NAD + (nicotinamide adenine dinucleotide) production, apoptosis-inducing ability and tumor cell killing ability, and higher infiltration into tumor tissues and tumor cell proliferation-inducing ability. CRC CD38 + NK cells also produce less TNF-alpha and more IL-2, ADO and TGF-beta. When the CD38 + NK cells were pretreated with anti-CD38 antibodies, the opposite results were obtained, and IFN-gamma production was increased. Wild-type C57BL/6 J mice grafted with mouse colon tumor-derived MC38 cells presented greater tumor growth, as well as higher Treg and CD38 + NK cell levels and lower Th1 cell levels in the peripheral blood than did the tumor-bearing model established with CD38 KO mice. Additionally, increased CD38, PD-1 and NF-kB expression and decreased CD16, Sirt1, Sirt6 and HSPA1 expression were detected in CRC CD38 + NK cells via real-time PCR and Western blot analysis, indicating that the NK cells expressed high CD38 and low CD16. High proportions of CD38 + CD16- NK cells were detected in the blood of CRC, GC, LC and OC patients. It is well known that high Tregs, TGF-beta, PD-1 and ADO levels, and low HSPA1, NAD + , TNF-alpha and IFN-gamma levels contribute to immune tumor cell escape. Our results suggest that a high proportion of CD38 (high) CD16 (low) NK cells in tumor patients can interrupt immune surveillance and favor tumor growth.

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Cancer immunology, immunotherapy : CII

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