Genetic alterations in CREBRF influence prostate cancer survival and impact prostate tissue homeostasis in mice.

IF 1.5 Q3 UROLOGY & NEPHROLOGY
Laura E Pascal, Krystle A Frahm, Kegan O Skalitzky, Donald B DeFranco, Lora H Rigatti, Ray Lu, Teresa T Liu
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引用次数: 0

Abstract

Background: Risk factors for prostate cancer include age, environment, race and ethnicity. Genetic variants in cyclic-adenosine-monophosphate-response-element-binding protein 3 regulatory factor (CREBRF) gene are frequently observed in Pacific Islanders, a population with elevated prostate cancer incidence. CREBRF has been shown to play a role in other cancers, however its function in prostate homeostasis and tumorigenesis has not been previously explored. We determined the incidence of CREBRF alterations in publicly available databases and examined the impact of CREBRF deletion on the murine prostate in order to determine whether CREBRF impacts prostate physiology or pathophysiology.

Methods: Alterations in CREBRF were identified in prostate cancer patients via in silico analysis of several publicly available datasets through cBioPortal. Male Crebrf knockout and wild-type littermate mice were generated and examined for prostate defects at 4 months of age. Immunohistochemical staining of murine prostate sections was used to determine the impact of Crebrf knockout on proliferation, apoptosis, inflammation and blood vessel density in the prostate. Serum adipokine levels were measured using a Luminex Multiplex Assay.

Results: CREBRF alterations were identified in up to 4.05% of prostate tumors and the mutations identified were categorized as likely damaging. Median survival of prostate cancer patients with genetic alterations in CREBRF was 41.23 months, compared to 131 months for patients without these changes. In the murine model, the prostates of Crebrf knockout mice had reduced epithelial proliferation and increased TUNEL+ apoptotic cells. Circulating adipokines PAI-1 and MCP-1 were also altered in Crebrf knockout mice compared to age-matched controls.

Conclusions: Prostate cancer patients with genetic alterations in CREBRF had a significantly decreased overall survival suggesting that wild type CREBRF may play a role in limiting prostate tumorigenesis and progression. The murine knockout model demonstrated that CREBRF could modulate proliferation and apoptosis and macrophage density in the prostate. Serum levels of adipokines PAI-1 and MCP-1 were also altered and may contribute to the phenotypic changes observed in the prostates of Crebrf knockout mice. Future studies focused on populations susceptible to CREBRF mutations and mechanistic studies will be required to fully elucidate the potential role of CREBRF in prostate tumorigenesis.

CREBRF的遗传改变影响前列腺癌存活并影响前列腺组织稳态。
背景:前列腺癌的危险因素包括年龄、环境、种族和民族。环腺苷-单磷酸-反应元件结合蛋白3调节因子(CREBRF)基因的遗传变异在太平洋岛民中经常被观察到,这是一个前列腺癌发病率高的人群。CREBRF已被证明在其他癌症中发挥作用,但其在前列腺稳态和肿瘤发生中的功能尚未被探索。我们在公开可用的数据库中确定了CREBRF改变的发生率,并检查了CREBRF缺失对小鼠前列腺的影响,以确定CREBRF是否影响前列腺生理或病理生理。方法:通过对几个公开数据集的计算机分析,在前列腺癌患者中确定CREBRF的改变。雄性Crebrf基因敲除小鼠和野生型同窝小鼠在4个月大时进行前列腺缺陷检查。采用小鼠前列腺切片免疫组化染色,检测Crebrf基因敲除对前列腺细胞增殖、凋亡、炎症和血管密度的影响。采用Luminex多重检测法测定血清脂肪因子水平。结果:在高达4.05%的前列腺肿瘤中发现了CREBRF改变,所发现的突变被归类为可能具有破坏性。CREBRF基因改变的前列腺癌患者的中位生存期为41.23个月,而没有这些改变的患者的中位生存期为131个月。在小鼠模型中,Crebrf基因敲除小鼠的前列腺上皮细胞增殖减少,TUNEL+凋亡细胞增加。与年龄匹配的对照组相比,Crebrf基因敲除小鼠的循环脂肪因子PAI-1和MCP-1也发生了改变。结论:CREBRF基因改变的前列腺癌患者总生存率显著降低,提示野生型CREBRF可能在限制前列腺肿瘤发生和进展方面发挥作用。小鼠敲除模型表明,CREBRF可以调节前列腺内巨噬细胞的增殖、凋亡和密度。血清中脂肪因子PAI-1和MCP-1的水平也发生了改变,这可能导致Crebrf基因敲除小鼠前列腺中观察到的表型变化。未来的研究将集中在对CREBRF突变易感的人群和机制研究上,以充分阐明CREBRF在前列腺肿瘤发生中的潜在作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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