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肿瘤免疫评估:来自种族匹配的军事队列的研究表明,肥大细胞耗竭可作为前列腺癌进展的标志物。

Immunologic Assessment of Tumors from a Race-matched Military Cohort Identifies Mast Cell Depletion as a Marker of Prostate Cancer Progression.

机构信息

Center for Prostate Disease Research, Murtha Cancer Center Research Program, Department of Surgery, Uniformed Services University of the Health Sciences, Bethesda, Maryland.

Henry M. Jackson Foundation for the Advancement of Military Medicine, Inc., Bethesda, Maryland.

出版信息

Cancer Res Commun. 2023 Aug 1;3(8):1423-1434. doi: 10.1158/2767-9764.CRC-22-0463. eCollection 2023 Aug.

Abstract

UNLABELLED

Elucidating the cellular immune components underlying aggressive prostate cancer, especially among African American (AA) men who are disproportionately affected by this disease compared with Caucasian American (CA) men, will support more inclusive precision medicine treatment strategies. We aimed to evaluate which immune-related genes and cell types are differentially expressed in AA tumors and how immunobiology impacts prostate cancer progression. We purified nucleic acid from tumor biopsies, obtained following radical prostatectomy, from 51 patients (AA = 26, CA = 25). Gene expression was measured using the NanoString platform from which we estimated immune cell abundances and assessed differences between groups based on clinicopathologic data. Product-limit estimates determined associations with biochemical recurrence (BCR)-free and metastasis-free survival. and were significantly upregulated in CA tumors and were also associated with worse disease progression. No significant differences in immune cell abundances by race were observed. Highly significant reductions in abundances of mast cells versus tumor-infiltrating lymphocytes (TIL) were found in men with high-grade pathologies and in men who later developed metastases. Low ratios of mast cells versus TILs were associated with worse BCR-free survival and metastasis-free survival. Although estimated immune cell abundances were not different by race, we identified genes involved in metabolism and natural killer cell functions that were differentially expressed between AA and CA tumors. Among the entire cohort, depletion of mast cells within prostatectomy tumors was characteristic of advanced disease and susceptibility to disease progression.

SIGNIFICANCE

Our findings demonstrate that there are immune-related genes and pathways that differ by race. Impaired intratumoral cellular immune composition, especially for TIL-normalized mast cells, may be vital in predicting and contributing to prostate cancer disease progression.

摘要

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阐明导致侵袭性前列腺癌的细胞免疫成分,特别是在非裔美国人(AA)男性中,因为与白种人(CA)男性相比,他们受到这种疾病的影响不成比例,这将支持更具包容性的精准医学治疗策略。我们旨在评估哪些免疫相关基因和细胞类型在 AA 肿瘤中表达不同,以及免疫生物学如何影响前列腺癌的进展。我们从 51 名接受根治性前列腺切除术的患者的肿瘤活检中提取了核酸(AA=26,CA=25)。我们使用 NanoString 平台测量了基因表达,该平台估计了免疫细胞的丰度,并根据临床病理数据评估了组间的差异。产品限制估计确定了与生化复发(BCR)无进展和无转移生存的关联。在 CA 肿瘤中, 和 显著上调,并且与疾病进展不良相关。未观察到按种族划分的免疫细胞丰度存在显着差异。在具有高级病理和后来发生转移的男性中,发现肥大细胞相对于肿瘤浸润淋巴细胞(TIL)的丰度显着降低。肥大细胞与 TIL 的低比例与 BCR 无进展生存和无转移生存不良相关。尽管按种族划分的估计免疫细胞丰度没有差异,但我们确定了参与代谢和自然杀伤细胞功能的基因在 AA 和 CA 肿瘤之间表达不同。在整个队列中,前列腺切除术肿瘤内肥大细胞的耗竭是疾病进展和疾病进展易感性的特征。

意义

我们的发现表明存在与种族相关的免疫相关基因和途径。肿瘤内细胞免疫组成的受损,特别是对于 TIL 归一化的肥大细胞,可能对预测和促进前列腺癌疾病进展至关重要。

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