CD38在前列腺癌中发生甲基化并调节细胞外烟酰胺腺嘌呤二核苷酸。
CD38 is methylated in prostate cancer and regulates extracellular NAD.
作者信息
Mottahedeh Jack, Haffner Michael C, Grogan Tristan R, Hashimoto Takao, Crowell Preston D, Beltran Himisha, Sboner Andrea, Bareja Rohan, Esopi David, Isaacs William B, Yegnasubramanian Srinivasan, Rettig Matthew B, Elashoff David A, Platz Elizabeth A, De Marzo Angelo M, Teitell Michael A, Goldstein Andrew S
机构信息
1Department of Molecular, Cell & Developmental Biology, University of California Los Angeles, Los Angeles, CA USA.
2Sidney Kimmel Comprehensive Cancer Center at Johns Hopkins, Baltimore, MD USA.
出版信息
Cancer Metab. 2018 Sep 21;6:13. doi: 10.1186/s40170-018-0186-3. eCollection 2018.
BACKGROUND
Cancer cell metabolism requires sustained pools of intracellular nicotinamide adenine dinucleotide (NAD) which is maintained by a balance of NAD hydrolase activity and NAD salvage activity. We recently reported that human prostate cancer can be initiated following oncogene expression in progenitor-like luminal cells marked by low expression of the NAD-consuming enzyme CD38. CD38 expression is reduced in prostate cancer compared to benign prostate, suggesting that tumor cells may reduce CD38 expression in order to enhance pools of NAD. However, little is known about how CD38 expression is repressed in advanced prostate cancer and whether CD38 plays a role in regulating NAD levels in prostate epithelial cells.
METHODS
CD38 expression, its association with recurrence after prostatectomy for clinically localized prostate cancer, and DNA methylation of the CD38 promoter were evaluated in human prostate tissues representing various stages of disease progression. CD38 was inducibly over-expressed in benign and malignant human prostate cell lines in order to determine the effects on cell proliferation and levels of NAD and NADH. NAD and NADH were also measured in urogenital tissues from wild-type and CD38 knockout mice.
RESULTS
CD38 mRNA expression was reduced in metastatic castration-resistant prostate cancer compared to localized prostate cancer. In a large cohort of men undergoing radical prostatectomy, CD38 protein expression was inversely correlated with recurrence. We identified methylation of the CD38 promoter in primary and metastatic prostate cancer. Over-expression of wild-type CD38, but not an NAD hydrolase-deficient mutant, depleted extracellular NAD levels in benign and malignant prostate cell lines. However, expression of CD38 did not significantly alter intracellular NAD levels in human prostate cell lines grown in vitro and in urogenital tissues isolated from wild-type and CD38 knockout mice.
CONCLUSIONS
CD38 protein expression in prostate cancer is associated with risk of recurrence. Methylation results suggest that CD38 is epigenetically regulated in localized and metastatic prostate cancer tissues. Our study provides support for CD38 as a regulator of extracellular, but not intracellular, NAD in epithelial cells. These findings suggest that repression of CD38 by methylation may serve to increase the availability of extracellular NAD in prostate cancer tissues.
背景
癌细胞代谢需要持续的细胞内烟酰胺腺嘌呤二核苷酸(NAD)池,其通过NAD水解酶活性和NAD补救活性的平衡来维持。我们最近报道,在以消耗NAD的酶CD38低表达为特征的祖细胞样管腔细胞中癌基因表达后,可引发人类前列腺癌。与良性前列腺相比,前列腺癌中CD38表达降低,这表明肿瘤细胞可能会降低CD38表达以增加NAD池。然而,关于晚期前列腺癌中CD38表达如何被抑制以及CD38是否在调节前列腺上皮细胞中NAD水平方面发挥作用,我们知之甚少。
方法
在代表疾病进展不同阶段的人类前列腺组织中,评估CD38表达、其与临床局限性前列腺癌前列腺切除术后复发的关联以及CD38启动子的DNA甲基化情况。在良性和恶性人类前列腺细胞系中诱导性过表达CD38,以确定其对细胞增殖以及NAD和NADH水平的影响。还在野生型和CD38基因敲除小鼠的泌尿生殖组织中测量了NAD和NADH。
结果
与局限性前列腺癌相比,转移性去势抵抗性前列腺癌中CD38 mRNA表达降低。在一大群接受根治性前列腺切除术的男性中,CD38蛋白表达与复发呈负相关。我们在原发性和转移性前列腺癌中鉴定出CD38启动子的甲基化。野生型CD38而非NAD水解酶缺陷型突变体的过表达,使良性和恶性前列腺细胞系中的细胞外NAD水平降低。然而,在体外培养的人类前列腺细胞系以及从野生型和CD38基因敲除小鼠分离的泌尿生殖组织中,CD38的表达并未显著改变细胞内NAD水平。
结论
前列腺癌中CD38蛋白表达与复发风险相关。甲基化结果表明,CD38在局限性和转移性前列腺癌组织中受到表观遗传调控。我们的研究支持CD38作为上皮细胞中细胞外而非细胞内NAD的调节剂。这些发现表明,甲基化对CD38的抑制作用可能有助于增加前列腺癌组织中细胞外NAD的可用性。
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