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恒河猴黄体自发功能消退期间发生的基因表达动态变化。

Dynamic changes in gene expression that occur during the period of spontaneous functional regression in the rhesus macaque corpus luteum.

作者信息

Bogan Randy L, Murphy Melinda J, Hennebold Jon D

机构信息

Oregon Health and Science University, Oregon National Primate Research Center, 505 Northwest 185th Avenue, Beaverton, Oregon 97006.

出版信息

Endocrinology. 2009 Mar;150(3):1521-9. doi: 10.1210/en.2008-1201. Epub 2008 Oct 23.

Abstract

Luteolysis of the corpus luteum (CL) during nonfertile cycles involves a cessation of progesterone (P4) synthesis (functional regression) and subsequent structural remodeling. The molecular processes responsible for initiation of luteal regression in the primate CL are poorly defined. Therefore, a genomic approach was used to systematically identify differentially expressed genes in the rhesus macaque CL during spontaneous luteolysis. CL were collected before [d 10-11 after LH surge, mid-late (ML) stage] or during (d 14-16, late stage) functional regression. Based on P4 levels, late-stage CL were subdivided into functional-late (serum P4 > 1.5 ng/ml) and functionally regressed late (FRL) (serum P4 < 0.5 ng/ml) groups (n = 4 CL per group). Total RNA was isolated, labeled, and hybridized to Affymetrix genome microarrays that contain elements representing the entire rhesus macaque transcriptome. With the ML stage serving as the baseline, there were 681 differentially expressed transcripts (>2-fold change; P < 0.05) that could be categorized into three primary patterns of expression: 1) increasing from ML through FRL; 2) decreasing from ML through FRL; and 3) increasing ML to functional late, followed by a decrease in FRL. Ontology analysis revealed potential mechanisms and pathways associated with functional and/or structural regression of the macaque CL. Quantitative real-time PCR was used to validate microarray expression patterns of 13 genes with the results being consistent between the two methodologies. Protein levels were found to parallel mRNA profiles in four of five differentially expressed genes analyzed by Western blot. Thus, this database will facilitate the identification of mechanisms involved in primate luteal regression.

摘要

非受孕周期中黄体(CL)的黄体溶解涉及孕酮(P4)合成的停止(功能衰退)以及随后的结构重塑。灵长类动物黄体中启动黄体退化的分子过程尚不清楚。因此,采用基因组学方法系统地鉴定恒河猴黄体在自发黄体溶解过程中差异表达的基因。在促黄体生成素峰后第10 - 11天(中期 - 晚期阶段)之前或功能衰退期间(第14 - 16天,晚期阶段)收集黄体。根据P4水平,将晚期黄体细分为功能晚期(血清P4 > 1.5 ng/ml)和功能衰退晚期(FRL)(血清P4 < 0.5 ng/ml)组(每组n = 4个黄体)。分离、标记总RNA,并与包含代表整个恒河猴转录组元件的Affymetrix基因组微阵列杂交。以中期 - 晚期阶段为基线,有681个差异表达的转录本(变化>2倍;P < 0.05),可分为三种主要表达模式:1)从中期 - 晚期到功能衰退晚期增加;2)从中期 - 晚期到功能衰退晚期减少;3)从中期 - 晚期增加到功能晚期,随后在功能衰退晚期减少。本体分析揭示了与猕猴黄体功能和/或结构衰退相关的潜在机制和途径。使用定量实时PCR验证13个基因的微阵列表达模式,两种方法的结果一致。通过蛋白质印迹分析的五个差异表达基因中的四个,发现蛋白质水平与mRNA谱平行。因此,该数据库将有助于识别灵长类动物黄体退化所涉及的机制。

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