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建立并鉴定三种人眼附属器皮脂腺癌细胞系。

Establishment and Characterization of Three Human Ocular Adnexal Sebaceous Carcinoma Cell Lines.

机构信息

Department of Pathology, The Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.

Department of Comparative Pathobiology, Tufts University Cummings School of Veterinary Medicine, North Grafton, MA 01536, USA.

出版信息

Int J Mol Sci. 2024 Sep 23;25(18):10183. doi: 10.3390/ijms251810183.

Abstract

Ocular adnexal sebaceous carcinoma (SebCA) represents one of the most clinically problematic periocular tumors, often requiring aggressive surgical resection. The pathobiology of this tumor remains poorly understood, and few models exist that are suitable for preclinical testing. The aim of this study was to establish new cell lines to serve as models for pathobiological and drug testing. With patient consent, freshly resected tumor tissue was cultured using conditional reprogramming cell conditions. Standard techniques were used to characterize the cell lines in terms of overall growth, clonogenicity, apoptosis, and differentiation in vitro. Additional analyses including Western blotting, short tandem repeat (STR) profiling, and next-generation sequencing (NGS) were performed. Drug screening using mitomycin-C (MMC), 5-fluorouricil (5-FU), and 6-Diazo-5-oxo-L-norleucine (DON) were performed. JHH-SebCA01, JHH-SebCA02, and JHH-SebCA03 cell lines were established from two women and one man undergoing surgical resection of eyelid tumors. At passage 15, they each showed a doubling time of two to three days, and all could form colonies in anchorage-dependent conditions, but not in soft agar. The cells contained cytoplasmic vacuoles consistent with sebaceous differentiation, and adipophilin protein was present in all three lines. STR profiling confirmed that all lines were derived from their respective patients. NGS of the primary tumors and their matched cell lines identified numerous shared mutations, including alterations similar to those previously described in SebCA. Treatment with MMC or 5-FU resulted in dose-dependent growth inhibition and the induction of both apoptosis and differentiation. MYC protein was abundant in all three lines, and the glutamine metabolism inhibitor DON, previously shown to target high MYC tumors, slowed the growth of all our SebCA models. Ocular adnexal SebCA cell lines can be established using conditional reprogramming cell conditions, and our three new models are useful for testing therapies and interrogating the functional role of MYC and other possible molecular drivers. Current topical chemotherapies promote both apoptosis and differentiation in SebCA cells, and these tumors appear sensitive to inhibition or MYC-associated metabolic changes.

摘要

眼附属器皮脂腺癌(SebCA)是临床最具挑战性的眼周肿瘤之一,常需行积极的手术切除。该肿瘤的病理生物学特性仍知之甚少,目前仅有少数适合于临床前检测的模型。本研究旨在建立新的细胞系,作为病理生物学和药物检测的模型。在患者知情同意的情况下,使用条件重编程细胞条件培养新鲜切除的肿瘤组织。采用标准技术从总体生长、集落形成能力、凋亡和体外分化等方面对细胞系进行特征描述。还进行了包括 Western blot、短串联重复序列(STR)分析和下一代测序(NGS)在内的额外分析。使用丝裂霉素 C(MMC)、5-氟尿嘧啶(5-FU)和 6-重氮-5-氧-L-正亮氨酸(DON)进行药物筛选。从两名女性和一名男性接受眼睑肿瘤切除术的患者中建立了 JHH-SebCA01、JHH-SebCA02 和 JHH-SebCA03 细胞系。在第 15 代时,它们的倍增时间均为两天至三天,并且所有细胞都可以在锚定依赖性条件下形成集落,但不能在软琼脂中形成。这些细胞含有与皮脂腺分化一致的细胞质空泡,并且所有三种细胞系中均存在脂肪蛋白。STR 分析证实所有细胞系均来自各自的患者。原发肿瘤及其匹配的细胞系的 NGS 鉴定出许多共同的突变,包括与 SebCA 中先前描述的相似的改变。用 MMC 或 5-FU 处理会导致剂量依赖性的生长抑制,并诱导凋亡和分化。所有三种细胞系中都有丰富的 MYC 蛋白,先前被证明靶向高 MYC 肿瘤的谷氨酰胺代谢抑制剂 DON 也减缓了我们所有 SebCA 模型的生长。眼附属器 SebCA 细胞系可以使用条件重编程细胞条件建立,我们的三个新模型可用于测试治疗方法,并研究 MYC 和其他可能的分子驱动因素的功能作用。目前的局部化疗药物可促进 SebCA 细胞的凋亡和分化,这些肿瘤似乎对抑制或与 MYC 相关的代谢变化敏感。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a06d/11432008/57d7feddc512/ijms-25-10183-g001.jpg

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