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新辅助化疗与胰腺导管腺癌中以 B 细胞为中心的免疫景观抑制有关。

Neoadjuvant chemotherapy is associated with suppression of the B cell-centered immune landscape in pancreatic ductal adenocarcinoma.

机构信息

Institute of Immunology, Faculty of Medicine Carl Gustav Carus, Technical University Dresden, Dresden, Germany.

Department of Surgery, Klinikum rechts der Isar, Technical University of Munich, Munich, Germany.

出版信息

Front Immunol. 2024 Apr 2;15:1378190. doi: 10.3389/fimmu.2024.1378190. eCollection 2024.

DOI:10.3389/fimmu.2024.1378190
PMID:38629072
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11018975/
Abstract

Pancreatic ductal adenocarcinoma (PDAC) is typically diagnosed at advanced stages and associated with early distant metastasis and poor survival. Besides clinical factors, the tumor microenvironment (TME) emerged as a crucial determinant of patient survival and therapy response in many tumors, including PDAC. Thus, the presence of tumor-infiltrating lymphocytes and the formation of tertiary lymphoid structures (TLS) is associated with longer survival in PDAC. Although neoadjuvant therapy (NeoTx) has improved the management of locally advanced tumors, detailed insight into its effect on various TME components is limited. While a remodeling towards a proinflammatory state was reported for PDAC-infiltrating T cells, the effect of NeoTx on B cell subsets, including plasma cells, and TLS formation is widely unclear. We thus investigated the frequency, composition, and spatial distribution of PDAC-infiltrating B cells in primary resected (PR) versus neoadjuvant-treated patients using a novel multiplex immunohistochemistry panel. The NeoTx group displayed significantly lower frequencies of pan B cells, GC B cells, plasmablasts, and plasma cells, accompanied by a reduced abundance of TLS. This finding was supported by bulk RNA-sequencing analysis of an independent fresh frozen tissue cohort, which revealed that major B cell pathways were downregulated in the NeoTx group. We further observed that plasma cells frequently formed aggregates that localized close to TLS and that TLS patients displayed significantly higher plasma cell frequencies compared to TLS patients in the PR group. Additionally, high densities of CD20 intratumoral B cells were significantly associated with longer overall survival in the PR group. While CD20 B cells held no prognostic value for NeoTx patients, an increased frequency of proliferating CD20Ki67 B cells emerged as an independent prognostic factor for longer survival in the NeoTx group. These results indicate that NeoTx differentially affects PDAC-infiltrating immune cells and may have detrimental effects on the existing B cell landscape and the formation of TLS. Gaining further insight into the underlying molecular mechanisms is crucial to overcome the intrinsic immunotherapy resistance of PDAC and develop novel strategies to improve the long-term outcome of PDAC patients.

摘要

胰腺导管腺癌 (PDAC) 通常在晚期诊断,且早期就发生远处转移,生存预后较差。除临床因素外,肿瘤微环境 (TME) 已成为许多肿瘤包括 PDAC 患者生存和治疗反应的重要决定因素。因此,肿瘤浸润淋巴细胞的存在和三级淋巴结构 (TLS) 的形成与 PDAC 患者的生存时间延长相关。虽然新辅助治疗 (NeoTx) 改善了局部晚期肿瘤的治疗管理,但对其对各种 TME 成分的影响的详细了解仍有限。虽然 PDAC 浸润 T 细胞的重塑向促炎状态发展,但 NeoTx 对包括浆细胞在内的 B 细胞亚群和 TLS 形成的影响尚不清楚。因此,我们使用新型多重免疫组化试剂盒研究了原发性切除 (PR) 与新辅助治疗患者的 PDAC 浸润 B 细胞的频率、组成和空间分布。NeoTx 组的 pan B 细胞、GC B 细胞、浆母细胞和浆细胞频率显著降低,同时 TLS 减少。这一发现得到了独立新鲜冷冻组织队列的批量 RNA 测序分析的支持,该分析显示,主要的 B 细胞途径在 NeoTx 组中下调。我们进一步观察到浆细胞经常形成聚集物,靠近 TLS 定位,且 TLS 患者的浆细胞频率明显高于 PR 组的 TLS 患者。此外,肿瘤内 CD20 浸润 B 细胞的高密度与 PR 组患者的总生存期延长显著相关。虽然 CD20 B 细胞对 NeoTx 患者没有预后价值,但增殖性 CD20Ki67 B 细胞的频率增加成为 NeoTx 组生存时间延长的独立预后因素。这些结果表明,NeoTx 对 PDAC 浸润免疫细胞有不同的影响,可能对现有的 B 细胞景观和 TLS 的形成产生不利影响。深入了解潜在的分子机制对于克服 PDAC 的固有免疫治疗抵抗并开发改善 PDAC 患者长期预后的新策略至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/434a/11018975/ed66603f4a4d/fimmu-15-1378190-g009.jpg
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