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照射可增强前列腺小细胞癌异种移植瘤的转移潜能。

Irradiation enhances the metastatic potential of prostatic small cell carcinoma xenografts.

作者信息

Agemy Lilach, Harmelin Alon, Waks Tova, Leibovitch Ilan, Rabin Tatyana, Pfeffer M Raphael, Eshhar Zelig

机构信息

Department of Immunology, The Weizmann Institute of Science, Rehovot, Israel.

出版信息

Prostate. 2008 Apr 1;68(5):530-9. doi: 10.1002/pros.20702.

Abstract

BACKGROUND

Small cell carcinoma of the prostate (SCCP) is a rare subset of prostate cancer (0.5-2% of all prostatic carcinomas), predominantly composed of neuroendocrine (NE) cells, with a very poor prognosis. Irradiation is one of the mainstay options for SCCP local treatment, yet, little is known about the clinical response of these aggressive tumors to radiotherapy.

METHODS

Using SCID mice, the response to fractionated ionizing radiation (IR) of two unique human NE xenografts of SCCP (WISH-PC2 and WM-4A) was investigated.

RESULTS

Fractionated irradiation of WISH-PC2 xenografts using total doses of >24 Gy induced a delay in tumor growth, while total doses of >36 Gy led to local tumor eradication. However, most of the irradiated mice suffered from disseminated metastases. Similarly, in the WM-4A xenograft, a total dose of 20 Gy led to tumor growth delay and some of the mice also developed metastases. Non-irradiated local xenografts failed to disseminate, even following surgical excision of the main tumor mass; however, tumor cells administered intravenously did form metastases. Metastases of both xenografts were located in the adrenal/kidney and inter-scapular regions, areas rich in brown adipose tissue. A correlation was found between the appearance of irradiation-induced metastases and activation of the gelatinase activity of matrix metalloproteinase-9.

CONCLUSIONS

Clinically, this study raises the possibility that radiation to SCCP may promote metastatic disease. For patients in whom prostate biopsy shows a predominance of small cell cancer, it may be necessary to deliver systemic therapy together with the radiotherapy in order to prevent the development of metastases.

摘要

背景

前列腺小细胞癌(SCCP)是前列腺癌中罕见的一种亚型(占所有前列腺癌的0.5 - 2%),主要由神经内分泌(NE)细胞组成,预后极差。放疗是SCCP局部治疗的主要选择之一,然而,对于这些侵袭性肿瘤对放疗的临床反应知之甚少。

方法

使用严重联合免疫缺陷(SCID)小鼠,研究了两种独特的人SCCP神经内分泌异种移植瘤(WISH - PC2和WM - 4A)对分次电离辐射(IR)的反应。

结果

对WISH - PC2异种移植瘤进行分次照射,总剂量>24 Gy可导致肿瘤生长延迟,而总剂量>36 Gy可导致局部肿瘤根除。然而,大多数接受照射的小鼠出现了广泛转移。同样,在WM - 4A异种移植瘤中,总剂量20 Gy导致肿瘤生长延迟,一些小鼠也出现了转移。未照射的局部异种移植瘤即使在手术切除主要肿瘤块后也未发生转移;然而,静脉注射的肿瘤细胞确实形成了转移灶。两种异种移植瘤的转移灶都位于肾上腺/肾脏和肩胛间区域,这些区域富含棕色脂肪组织。发现辐射诱导的转移灶的出现与基质金属蛋白酶-9的明胶酶活性的激活之间存在相关性。

结论

在临床上,本研究提出了SCCP放疗可能促进转移性疾病的可能性。对于前列腺活检显示小细胞癌占优势的患者,可能有必要在放疗的同时进行全身治疗,以防止转移的发生。

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