{"title":"急性髓系白血病中粘附性gpcr上调的表征。","authors":"Jiawen Yang, Sharon K. Wu, Houda Alachkar","doi":"10.1182/BLOOD-2018-99-119998","DOIUrl":null,"url":null,"abstract":"The role of adhesion G protein-coupled receptors (aGPCRs) in cancer has become increasingly evident in recent years. Yet, data supporting the contribution of this family of genes to hematological malignancies, particularly acute myeloid leukemia (AML) are limited. Here, we use publicly available genomic data to characterize the expression of the 33 aGPCRs in patients with AML and examine whether upregulation of these genes is associated with the clinical and molecular characteristics of patients. Upregulation in one or more of eight aGPCR genes (ADGRB1, ADGRC2, ADGRD1, ADGRE1, ADGRE2, ADGRE5, ADGRG1, and/or ADGRG3) was significantly associated with shorter overall survival (OS) (median OS: 11.8 vs 55.4 months; P < 0.0001). This was also significant in multivariate survival analysis (hazard ratio: 1.73; 95% confidence interval 1.11-2.69; P = 0.015) after adjusting for age, molecular risk status, and transplant status. High expression of the eight aGPCRs was significantly associated with older age (≥60; P = 0.011). Patients with high aGPCRs expression were more frequently classified in the poor molecular risk status group and less in the good risk status group compared with patients with low aGPCRs expression (31% vs 17% P = 0.049 and 14% vs 28% P = 0.027, respectively). Via Ingenuity Pathway Analysis, we identified the interleukin-8 signaling pathway among the most activated pathways in patients with high aGPCRs expression. Overall, our data suggest that particular aGPCRs are frequently upregulated in AML and associated with poor clinical outcome. Future functional and mechanistic analyses are needed to address the role of aGPCRs in AML.","PeriodicalId":94257,"journal":{"name":"Translational research : the journal of laboratory and clinical medicine","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2018-11-21","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"9","resultStr":"{\"title\":\"Characterization of upregulated adhesion GPCRs in acute myeloid leukemia.\",\"authors\":\"Jiawen Yang, Sharon K. Wu, Houda Alachkar\",\"doi\":\"10.1182/BLOOD-2018-99-119998\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"The role of adhesion G protein-coupled receptors (aGPCRs) in cancer has become increasingly evident in recent years. Yet, data supporting the contribution of this family of genes to hematological malignancies, particularly acute myeloid leukemia (AML) are limited. Here, we use publicly available genomic data to characterize the expression of the 33 aGPCRs in patients with AML and examine whether upregulation of these genes is associated with the clinical and molecular characteristics of patients. Upregulation in one or more of eight aGPCR genes (ADGRB1, ADGRC2, ADGRD1, ADGRE1, ADGRE2, ADGRE5, ADGRG1, and/or ADGRG3) was significantly associated with shorter overall survival (OS) (median OS: 11.8 vs 55.4 months; P < 0.0001). This was also significant in multivariate survival analysis (hazard ratio: 1.73; 95% confidence interval 1.11-2.69; P = 0.015) after adjusting for age, molecular risk status, and transplant status. High expression of the eight aGPCRs was significantly associated with older age (≥60; P = 0.011). Patients with high aGPCRs expression were more frequently classified in the poor molecular risk status group and less in the good risk status group compared with patients with low aGPCRs expression (31% vs 17% P = 0.049 and 14% vs 28% P = 0.027, respectively). Via Ingenuity Pathway Analysis, we identified the interleukin-8 signaling pathway among the most activated pathways in patients with high aGPCRs expression. Overall, our data suggest that particular aGPCRs are frequently upregulated in AML and associated with poor clinical outcome. 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引用次数: 9
摘要
近年来,粘附G蛋白偶联受体(agpcr)在癌症中的作用越来越明显。然而,支持该基因家族对血液系统恶性肿瘤,特别是急性髓性白血病(AML)的贡献的数据有限。在这里,我们使用公开可用的基因组数据来表征AML患者中33种agpcr的表达,并检查这些基因的上调是否与患者的临床和分子特征相关。8个aGPCR基因(ADGRB1、ADGRC2、ADGRD1、ADGRE1、ADGRE2、ADGRE5、ADGRG1和/或ADGRG3)中的一个或多个基因上调与总生存期(OS)缩短显著相关(中位OS: 11.8 vs 55.4个月;P < 0.0001)。这在多变量生存分析中也是显著的(风险比:1.73;95%置信区间1.11-2.69;P = 0.015),在调整了年龄、分子危险状态和移植状态后。8种agpcr的高表达与老年显著相关(≥60;P = 0.011)。与agpcr低表达的患者相比,agpcr高表达的患者更常被归为不良分子风险状态组,而较低表达的患者更少被归为良好风险状态组(分别为31%对17% P = 0.049和14%对28% P = 0.027)。通过匠心通路分析,我们发现白细胞介素-8信号通路是agpcr高表达患者中最活跃的通路之一。总的来说,我们的数据表明,特定的agpcr在AML中经常上调,并与不良的临床结果相关。未来的功能和机制分析需要解决agpcr在AML中的作用。
Characterization of upregulated adhesion GPCRs in acute myeloid leukemia.
The role of adhesion G protein-coupled receptors (aGPCRs) in cancer has become increasingly evident in recent years. Yet, data supporting the contribution of this family of genes to hematological malignancies, particularly acute myeloid leukemia (AML) are limited. Here, we use publicly available genomic data to characterize the expression of the 33 aGPCRs in patients with AML and examine whether upregulation of these genes is associated with the clinical and molecular characteristics of patients. Upregulation in one or more of eight aGPCR genes (ADGRB1, ADGRC2, ADGRD1, ADGRE1, ADGRE2, ADGRE5, ADGRG1, and/or ADGRG3) was significantly associated with shorter overall survival (OS) (median OS: 11.8 vs 55.4 months; P < 0.0001). This was also significant in multivariate survival analysis (hazard ratio: 1.73; 95% confidence interval 1.11-2.69; P = 0.015) after adjusting for age, molecular risk status, and transplant status. High expression of the eight aGPCRs was significantly associated with older age (≥60; P = 0.011). Patients with high aGPCRs expression were more frequently classified in the poor molecular risk status group and less in the good risk status group compared with patients with low aGPCRs expression (31% vs 17% P = 0.049 and 14% vs 28% P = 0.027, respectively). Via Ingenuity Pathway Analysis, we identified the interleukin-8 signaling pathway among the most activated pathways in patients with high aGPCRs expression. Overall, our data suggest that particular aGPCRs are frequently upregulated in AML and associated with poor clinical outcome. Future functional and mechanistic analyses are needed to address the role of aGPCRs in AML.