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前列腺炎症对前列腺癌发生的POET3(+)Pten(+/-)小鼠模型中病变发展的影响。

Impact of prostate inflammation on lesion development in the POET3(+)Pten(+/-) mouse model of prostate carcinogenesis.

作者信息

Burcham Grant N, Cresswell Gregory M, Snyder Paul W, Chen Long, Liu Xiaoqi, Crist Scott A, Henry Michael D, Ratliff Timothy L

机构信息

Department of Comparative Pathobiology, College of Veterinary Medicine, Purdue University, West Lafayette, Indiana; Heeke Animal Disease Diagnostic Laboratory, Southern Indiana Purdue Agricultural Center, Dubois, Indiana.

Department of Comparative Pathobiology, College of Veterinary Medicine, Purdue University, West Lafayette, Indiana.

出版信息

Am J Pathol. 2014 Dec;184(12):3176-91. doi: 10.1016/j.ajpath.2014.08.021. Epub 2014 Nov 22.

Abstract

Evidence linking prostatitis and prostate cancer development is contradictory. To study this link, the POET3 mouse, an inducible model of prostatitis, was crossed with a Pten-loss model of prostate cancer (Pten(+/-)) containing the ROSA26 luciferase allele to monitor prostate size. Prostatitis was induced, and prostate bioluminescence was tracked over 12 months, with lesion development, inflammation, and cytokine expression analyzed at 4, 8, and 12 months and compared with mice without induction of prostatitis. Acute prostatitis led to more proliferative epithelium and enhanced bioluminescence. However, 4 months after initiation of prostatitis, mice with induced inflammation had lower grade pre-neoplastic lesions. A trend existed toward greater development of carcinoma 12 months after induction of inflammation, including one of two mice with carcinoma developing perineural invasion. Two of 18 mice at the later time points developed lesions with similarities to proliferative inflammatory atrophy, including one mouse with associated carcinoma. Pten(+/-) mice developed spontaneous inflammation, and prostatitis was similar among groups of mice at 8 and 12 months. Analyzed as one cohort, lesion number and grade were positively correlated with prostatitis. Specifically, amounts of CD11b(+)Gr1(+) cells were correlated with lesion development. These results support the hypothesis that myeloid-based inflammation is associated with lesion development in the murine prostate, and previous bouts of CD8-driven prostatitis may promote invasion in the Pten(+/-) model of cancer.

摘要

将前列腺炎与前列腺癌发展联系起来的证据相互矛盾。为了研究这种联系,将POET3小鼠(一种可诱导的前列腺炎模型)与含有ROSA26荧光素酶等位基因的前列腺癌Pten缺失模型(Pten(+/-))杂交,以监测前列腺大小。诱导产生前列腺炎,并在12个月内追踪前列腺生物发光情况,在4个月、8个月和12个月时分析病变发展、炎症和细胞因子表达,并与未诱导前列腺炎的小鼠进行比较。急性前列腺炎导致上皮细胞增殖增加和生物发光增强。然而,在前列腺炎开始后的4个月,诱导炎症的小鼠的癌前病变级别较低。在炎症诱导12个月后,存在癌发展增加的趋势,包括两只患癌小鼠中有一只发生神经周围浸润。在后期时间点,18只小鼠中有两只出现了与增殖性炎性萎缩相似的病变,其中一只伴有癌。Pten(+/-)小鼠发生自发性炎症,在8个月和12个月时各小鼠组之间的前列腺炎情况相似。作为一个队列进行分析,病变数量和级别与前列腺炎呈正相关。具体而言,CD11b(+)Gr1(+)细胞的数量与病变发展相关。这些结果支持这样的假设,即基于髓系的炎症与小鼠前列腺中的病变发展相关,并且先前由CD8驱动的前列腺炎发作可能会促进Pten(+/-)癌症模型中的侵袭。

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