Dongyun Zhang, Willy Hugo, Marvin Bergsneider, Marilene B Wang, Won Kim, Karam Han, Harry V Vinters, Anthony P Heaney
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Tumor cells from CBG-treated patients expressed lower levels of genes that regulated hormone secretion, such as SCG2, VGF, TIMP1, NNAT, and CALD1, consistent with the inhibitory effects of CBG on hormone processing and secretion. Interestingly, we also observed an increased number of CD8+ T cells in the CBG-treated tissues. These cytotoxic CD8+ T cells expressed killing granule components such as perforin and the granzymes GZMB, GNLY, and KLRD1 as well as the inflammatory cytokine CCL5. Immune cell activation of these CD8+ T cells was further analyzed in a compartment-specific manner, and increased CD25 (IL2R) expression was noted in the CD8+ T cells from the CBG-treated samples. 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引用次数: 0
摘要
目的:揭示多巴胺激动剂疗法在人类催乳素瘤及其邻近基质和免疫细胞中的靶上和靶下作用的潜在机制:揭示多巴胺受体激动剂治疗在人类泌乳素瘤肿瘤及邻近基质细胞和免疫细胞中的靶上和靶下作用的潜在机制:通过单细胞RNA测序(scRNA-seq)分析了3名接受过卡贝戈林(CBG)治疗的患者和2名未接受过治疗的患者的5个手术切除的泌乳素瘤,以比较细胞组成和转录情况:观察到六种主要细胞群,包括肿瘤细胞(88.2%)、免疫细胞(5.6%)、基质细胞(4.9%)、祖细胞(0.6%)、增殖细胞(0.4%)和红细胞(0.2%)。经 CBG 治疗的患者的肿瘤细胞表达了较低水平的激素分泌调控基因,如 SCG2、VGF、TIMP1、NNAT 和 CALD1,这与 CBG 对激素加工和分泌的抑制作用是一致的。有趣的是,我们还在 CBG 处理过的组织中观察到 CD8+ T 细胞数量的增加。这些细胞毒性 CD8+ T 细胞表达杀伤性颗粒成分,如穿孔素、颗粒酶 GZMB、GNLY 和 KLRD1 以及炎性细胞因子 CCL5。研究人员进一步分析了这些 CD8+ T 细胞的免疫细胞活化情况,发现 CBG 处理样本的 CD8+ T 细胞中 CD25(IL2R)表达增加。此外,我们还注意到,CBG 处理的样本中基质细胞数量较多,这也证实了之前的报道:我们的 scRNAseq 研究揭示了 CBG 处理过的 PRLomas 与未处理过的 PRLomas 在肿瘤和微环境细胞成分方面的转录组特征的关键差异,并首次描述了之前未知的 CD8+ T 细胞在 CBG 处理后的活化,这可能在 CBG 的杀瘤作用中发挥作用。
Cabergoline targets multiple pathways to inhibit PRL secretion and increases stromal fibrosis.
Objective: Unravel the potential mechanism(s) of the on- and off-target actions of dopamine agonist therapy in both human prolactinoma tumors and neighboring stromal and immune cells.
Design and methods: Five surgically resected prolactinomas (PRLomas) from 3 cabergoline (CBG)-treated patients and 2 treatment-naive patients were analyzed by using single-cell RNA sequencing (scRNA-seq) to compare the cellular composition and transcriptional landscape.
Results: Six major cell populations, namely tumor (88.2%), immune (5.6%), stromal (4.9%), progenitor cells (0.6%), proliferating cells (0.4%), and erythrocytes (0.2%), were observed. Tumor cells from CBG-treated patients expressed lower levels of genes that regulated hormone secretion, such as SCG2, VGF, TIMP1, NNAT, and CALD1, consistent with the inhibitory effects of CBG on hormone processing and secretion. Interestingly, we also observed an increased number of CD8+ T cells in the CBG-treated tissues. These cytotoxic CD8+ T cells expressed killing granule components such as perforin and the granzymes GZMB, GNLY, and KLRD1 as well as the inflammatory cytokine CCL5. Immune cell activation of these CD8+ T cells was further analyzed in a compartment-specific manner, and increased CD25 (IL2R) expression was noted in the CD8+ T cells from the CBG-treated samples. Additionally, and confirming prior reports, we noted a higher stromal cell population in the CBG-treated samples.
Conclusions: Our scRNA-seq studies revealed key differences in the transcriptomic features of CBG-treated and CBG-untreated PRLomas in both tumor and microenvironment cellular constituents, and for the first time, describe the previously unknown activation of CD8+ T cells following CBG treatment, which may play a role in the tumoricidal actions of CBG.
期刊介绍:
European Journal of Endocrinology is the official journal of the European Society of Endocrinology. Its predecessor journal is Acta Endocrinologica.
The journal publishes high-quality original clinical and translational research papers and reviews in paediatric and adult endocrinology, as well as clinical practice guidelines, position statements and debates. Case reports will only be considered if they represent exceptional insights or advances in clinical endocrinology.
Topics covered include, but are not limited to, Adrenal and Steroid, Bone and Mineral Metabolism, Hormones and Cancer, Pituitary and Hypothalamus, Thyroid and Reproduction. In the field of Diabetes, Obesity and Metabolism we welcome manuscripts addressing endocrine mechanisms of disease and its complications, management of obesity/diabetes in the context of other endocrine conditions, or aspects of complex disease management. Reports may encompass natural history studies, mechanistic studies, or clinical trials.
Equal consideration is given to all manuscripts in English from any country.