膀胱癌与重金属升高有关:通过线粒体功能障碍、氧化应激和丝裂原活化蛋白激酶调查可能的致癌途径。

Bedeir Ali-El-Dein, Mahmoud Abdelgawad, Mohamed Tarek, Mona Abdel-Rahim, Manar E Elkady, Hazem H Saleh, Mahmoud M Zakaria, Heba H Tarabay, Mahmoud Laymon, Ahmed Mosbah, Arnolf Stenzl
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引用次数: 0

摘要

目的:重金属/微量元素(HMTE)在膀胱癌(BC)中的致癌机制尚不明确。线粒体功能障碍(MD)、氧化应激(OS)和丝裂原活化蛋白激酶(MAPK)是可能的致癌机制。本研究的目的是利用 6 个 MD 基因、7 个 OS 标记和 p38-MAPK 研究 BC 中 HMTE 的可能致癌途径:研究纳入了2020年10月至2022年10月期间的125例BC/根治性膀胱切除术(RC)患者和72例对照组。排除标准包括既往肿瘤、化疗或放疗。从 RC 标本中提取两种样本(癌症/非癌症)。组织/血浆/尿液中的镉 (Cd)、铅 (Pb)、钴 (Co)、镍 (Ni)、锶 (Sr)、铝 (Al)、锌 (Zn) 和硼 (B) 采用 ICP-OES 测量。组织 MD 基因(mt-CO3、mt-CYB、mt-ATP 6、mt-ATP8、mt-CO1、mt-ND1)和血清 OS 标志物(8-OHdG、MDA、3-NT、AGEs、AOPP、ROS、SOD2)、p38-MAPK 分别通过 RT-PCR 和 ELISA 进行评估:与对照组相比,BC 及其邻近组织中的铝、钴、铅、镍、锌、镉、锶浓度较高,硼浓度较低。高组织浓度(镉、钴、铅、镍、锶)与高MD基因、OS、MAPK和低SOD2水平相关。在 41 例同时伴有两种或两种以上 HMTE 升高的患者中,同样的差异更大。未纳入BC相关癌基因(如RAS)是一个限制因素:有证据表明,高浓度的BC组织(镉、钴、铅、镍、硅)与过度表达的MD基因、OS、p38-MAPK和低SOD2有关。这些发现为了解与 HMTE 相关的 BC 可能的致癌途径提供了重要依据。因此,应尽量减少和抵制接触有毒的 HMTE。
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Bladder cancer associated with elevated heavy metals: Investigation of probable carcinogenic pathways through mitochondrial dysfunction, oxidative stress and mitogen-activated protein kinase.

Objective: Carcinogenic mechanisms of heavy metals/ trace elements (HMTE) in bladder cancer (BC) are exactly unknown. Mitochondrial dysfunction (MD), oxidative stress (OS), and mitogen-activated protein kinases (MAPK) are probable carcinogenic mechanisms. The purpose is to investigate probable carcinogenic pathways of HMTE in BC using six MD genes, seven OS markers, and p38-MAPK.

Methods: Study included 125 BC/radical cystectomy (RC) patients between October 2020 and October 2022, and 72 controls. Exclusion criteria included previous neoplasm, chemo- or radiotherapy. Two samples (cancer/noncancer) were taken from RC specimens. Tissues/plasma/urine cadmium (Cd), lead (Pb), cobalt (Co), nickel (Ni), strontium (Sr), aluminium (Al), zinc (Zn), boron (B) were measured by ICP-OES. Tissue MD genes (mt-CO3, mt-CYB, mt-ATP 6, mt-ATP8, mt-CO1, mt-ND1), and serum OS markers (8-OHdG, MDA, 3-NT, AGEs, AOPP, ROS, SOD2), p38-MAPK were assessed by RT-PCR, and ELISA, respectively.

Results: BC and adjacent tissue showed higher (Al, Co, Pb, Ni, Zn, Cd,Sr), lower B concentrations, compared to controls. High tissue concentrations (Cd, Co, Pb, Ni, Sr) were associated with higher MD genes, OS, MAPK and lower SOD2 levels. The same differences were greater in 41 patients with concomitant elevation of two or more HMTE. Noninclusion of BC-related oncogenes (e.g. RAS) is a limitation.

Conclusions: Evidence suggests that high BC tissue (Cd, Co, Pb, Ni, Si) concentrations are associated with over-expressed MD genes, OS, p38-MAPK and low SOD2. These findings provide important understanding keys of probable carcinogenic pathways in BC associated with HMTE. So, efforts should be performed to minimize and counteract exposure to toxic HMTE.

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来源期刊
CiteScore
4.80
自引率
3.70%
发文量
297
审稿时长
7.6 weeks
期刊介绍: Urologic Oncology: Seminars and Original Investigations is the official journal of the Society of Urologic Oncology. The journal publishes practical, timely, and relevant clinical and basic science research articles which address any aspect of urologic oncology. Each issue comprises original research, news and topics, survey articles providing short commentaries on other important articles in the urologic oncology literature, and reviews including an in-depth Seminar examining a specific clinical dilemma. The journal periodically publishes supplement issues devoted to areas of current interest to the urologic oncology community. Articles published are of interest to researchers and the clinicians involved in the practice of urologic oncology including urologists, oncologists, and radiologists.
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Editorial Board Table of Contents Cover 2 - Masthead Cover 3 - GF 397 Delayed partial nephrectomy following complete response to immunotherapy: feasibility and results (UroCCR n°157).
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