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膀胱癌治疗靶点。

Targets for Therapy of Bladder Cancer.

机构信息

Department of Nuclear Medicine, Klinikum rechts der Isar, Technische Universität München, München, Germany.

出版信息

Semin Nucl Med. 2020 Mar;50(2):162-170. doi: 10.1053/j.semnuclmed.2020.02.006. Epub 2020 Feb 29.

DOI:10.1053/j.semnuclmed.2020.02.006
PMID:32172801
Abstract

In 2018 bladder cancer (urothelial carcinoma) was ranked twelfth concerning worldwide diagnosis of malignancies. At the time point of diagnosis of bladder cancer, approximately 75% of patients present with a nonmuscle-invasive disease (NMIBC), while the remaining 25% show invasion of tumor cells in the muscle layer of the bladder wall (MIBC). Among NMIBC tumors, flat, high-grade carcinoma in situ (CIS) is a therapeutic challenge. CIS shows a tendency to invade the muscle tissue of the bladder wall and thus become a MIBC. Standard therapy of NMIBC (including CIS) is done via intravesical instillation of BCG (bacillus Calmette Guerin) inducing a local immune reaction that finally promotes elimination of bladder cancer cells. However, BCG treatment of NMIBC proves to be ineffective in approximately 40% of patients. Therefore, new therapeutic approaches for the treatment of bladder cancer are urgently needed. Among promising new treatment options that are currently being investigated are the use of immune checkpoint inhibitors, and targeted approaches attacking (among others) long noncoding RNAs, micro RNAs, cancer stem cells, PARP1, and receptor signaling pathways. Moreover, the use of antibody-drug-conjugates (ADCs) is investigated also in bladder cancer therapy. Another approach that has been successfully established in preclinical studies uses the cytotoxic power of the alpha-emitter Bi-213 coupled to an antibody targeting EGFR. Overexpression of EGFR has been demonstrated in the majority of patients suffering from CIS. Feasibility, safety, toxicity and therapeutic efficacy of intravesical instillation of Bi-213-anti-EGFR have been evaluated in a pilot study. Since the results of the pilot study proved to be promising, a further optimization of alpha-emitter immunotherapy in bladder cancer seems mandatory.

摘要

2018 年膀胱癌(尿路上皮癌)在全球恶性肿瘤诊断中排名第十二。在诊断膀胱癌时,约 75%的患者患有非肌肉浸润性疾病(NMIBC),而其余 25%的患者表现为肿瘤细胞侵犯膀胱壁的肌肉层(MIBC)。在 NMIBC 肿瘤中,扁平、高级别原位癌(CIS)是一个治疗挑战。CIS 有侵犯膀胱壁肌肉组织的倾向,从而成为 MIBC。NMIBC(包括 CIS)的标准治疗是通过膀胱内灌注卡介苗(BCG)进行的,这会引起局部免疫反应,最终促进膀胱癌细胞的消除。然而,BCG 治疗 NMIBC 在大约 40%的患者中无效。因此,迫切需要新的治疗膀胱癌的方法。目前正在研究的有前途的新治疗选择包括使用免疫检查点抑制剂,以及靶向攻击(包括)长链非编码 RNA、microRNAs、癌症干细胞、PARP1 和受体信号通路的方法。此外,抗体药物偶联物(ADCs)也被用于膀胱癌治疗。另一种在临床前研究中成功建立的方法是利用与针对 EGFR 的抗体偶联的α发射器 Bi-213 的细胞毒性。大多数 CIS 患者的 EGFR 表达过度。在一项初步研究中评估了膀胱内注射 Bi-213-抗 EGFR 的可行性、安全性、毒性和治疗效果。由于初步研究的结果很有希望,因此似乎有必要进一步优化膀胱癌的α发射器免疫疗法。

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