Institute of Pathology, University Medical Centre Mannheim and Medical Faculty Mannheim, Heidelberg University, Mannheim, Germany.
Diagnostic Pathology, Kyoto University Hospital, Kyoto, Japan.
Cell Death Dis. 2022 Nov 19;13(11):979. doi: 10.1038/s41419-022-05428-x.
Tuft cells are chemosensory epithelial cells in the respiratory tract and several other organs. Recent studies revealed tuft cell-like gene expression signatures in some pulmonary adenocarcinomas, squamous cell carcinomas (SQCC), small cell carcinomas (SCLC), and large cell neuroendocrine carcinomas (LCNEC). Identification of their similarities could inform shared druggable vulnerabilities. Clinicopathological features of tuft cell-like (tcl) subsets in various lung cancer histotypes were studied in two independent tumor cohorts using immunohistochemistry (n = 674 and 70). Findings were confirmed, and additional characteristics were explored using public datasets (RNA seq and immunohistochemical data) (n = 555). Drug susceptibilities of tuft cell-like SCLC cell lines were also investigated. By immunohistochemistry, 10-20% of SCLC and LCNEC, and approximately 2% of SQCC expressed POU2F3, the master regulator of tuft cells. These tuft cell-like tumors exhibited "lineage ambiguity" as they co-expressed NCAM1, a marker for neuroendocrine differentiation, and KRT5, a marker for squamous differentiation. In addition, tuft cell-like tumors co-expressed BCL2 and KIT, and tuft cell-like SCLC and LCNEC, but not SQCC, also highly expressed MYC. Data from public datasets confirmed these features and revealed that tuft cell-like SCLC and LCNEC co-clustered on hierarchical clustering. Furthermore, only tuft cell-like subsets among pulmonary cancers significantly expressed FOXI1, the master regulator of ionocytes, suggesting their bidirectional but immature differentiation status. Clinically, tuft cell-like SCLC and LCNEC had a similar prognosis. Experimentally, tuft cell-like SCLC cell lines were susceptible to PARP and BCL2 co-inhibition, indicating synergistic effects. Taken together, pulmonary tuft cell-like cancers maintain histotype-related clinicopathologic characteristics despite overlapping unique molecular features. From a therapeutic perspective, identification of tuft cell-like LCNECs might be crucial given their close kinship with tuft cell-like SCLC.
类簇细胞是呼吸道和其他几个器官中的化学感觉上皮细胞。最近的研究表明,在一些肺腺癌、鳞状细胞癌(SQCC)、小细胞癌(SCLC)和大细胞神经内分泌癌(LCNEC)中存在类簇细胞样基因表达特征。鉴定它们的相似性可以提供共同的可药物治疗的脆弱性。使用免疫组织化学(n=674 和 70)在两个独立的肿瘤队列中研究了各种肺癌组织型中的类簇细胞样(tcl)亚群的临床病理特征。通过免疫组织化学,在 10-20%的 SCLC 和 LCNEC 以及大约 2%的 SQCC 中表达了 POU2F3,这是簇细胞的主要调节因子。这些类簇细胞样肿瘤表现出“谱系模糊性”,因为它们共同表达了 NCAM1,这是神经内分泌分化的标志物,以及 KRT5,这是鳞状分化的标志物。此外,类簇细胞样肿瘤还共同表达了 BCL2 和 KIT,并且类簇细胞样 SCLC 和 LCNEC 但不是 SQCC 也高度表达了 MYC。来自公共数据集的数据证实了这些特征,并揭示了类簇细胞样 SCLC 和 LCNEC 在层次聚类上共同聚类。此外,只有在肺癌中,类簇细胞样亚群才显著表达 FOXI1,这是离子细胞的主要调节因子,表明它们具有双向但不成熟的分化状态。临床上,类簇细胞样 SCLC 和 LCNEC 具有相似的预后。实验上,类簇细胞样 SCLC 细胞系对 PARP 和 BCL2 联合抑制敏感,表明存在协同作用。总之,肺类簇细胞样癌症尽管具有重叠的独特分子特征,但仍保持与组织型相关的临床病理特征。从治疗的角度来看,由于类簇细胞样 LCNEC 与类簇细胞样 SCLC 密切相关,因此识别它们可能至关重要。
Zotero 插件