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Survival benefit of sphingosin‐1‐phosphate and receptors expressions in breast cancer patients

机译:鞘氨醇-1-磷酸及其受体表达对乳腺癌患者的生存益处

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摘要

Sphingosine‐1‐phosphate (S1P) is a bioactive lipid that exerts various pathophysiological functions through binding to its receptor family (S1PRs). Since first report of the breast cancer (BCA) promoting function by S1P production (through the function of sphingosine kinases) and S1P/S1PR signaling, their antagonists have never been successfully progress to clinics after three decades. Taking advantage of bioinformatics linking to gene expression to disease prognosis, we examined the impact of associated genes in BCA patients. We found high gene expressions involved in S1P anabolism suppressed disease progression of patients who are basal cell type BCA or receiving adjuvant therapy. In addition, S1PRs expression also suppressed disease progress of multiple categories of BCA patient progression. This result is contradictory to tumor promoter role of S1P/S1PRs which revealed in the literature. Further examination by directly adding S1P in BCA cells found a cell growth suppression function, which act via the expression of S1PR1. In conclusion, our study is the first evidence claiming a survival benefit function of S1P/S1PR signaling in BCA patients, which might explain the obstacle of relative antagonist apply in clinics.
机译:鞘氨醇-1-磷酸(S1P)是一种生物活性脂质,通过与受体家族(S1PRs)结合而发挥各种病理生理功能。自乳腺癌(BCA)通过S1P产生(通过鞘氨醇激酶的功能)促进功能和S1P / S1PR信号转导以来的首次报道以来,它们的拮抗剂在三十年后从未成功进入临床。利用与基因表达相关的生物信息学与疾病预后的联系,我们研究了相关基因对BCA患者的影响。我们发现参与S1P合成代谢的高基因表达抑制了基底细胞BCA型或接受辅助治疗的患者的疾病进展。此外,S1PRs的表达还抑制了多类BCA患者病情的进展。该结果与文献中揭示的S1P / S1PRs的肿瘤启动子作用相反。通过在BCA细胞中直接添加S1P进行进一步检查,发现细胞生长抑制功能通过S1PR1的表达发挥作用。总之,我们的研究是第一个声称BCA患者具有S1P / S1PR信号的生存受益功能的证据,这可能解释了相对拮抗剂在临床中应用的障碍。

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