Abstract

To unveil novel global changes associated with corpus luteum (CL) maturation, we analyzed transcriptome data for the bovine CL on days 4 and 11, representing the developing vs. mature gland. Our analyses revealed 681 differentially expressed genes (363 and 318 on day 4 and 11, respectively), with ≥2 fold change and FDR of <5%. Different gene ontology (GO) categories were represented prominently in transcriptome data at these stages (e.g. days 4: cell cycle, chromosome, DNA metabolic process and replication and on day 11: immune response; lipid metabolic process and complement activation). Based on bioinformatic analyses, select genes expression in day 4 and 11 CL was validated with quantitative real-time PCR. Cell specific expression was also determined in enriched luteal endothelial and steroidogenic cells. Genes related to the angiogenic process such as NOS3, which maintains dilated vessels and MMP9, matrix degrading enzyme, were higher on day 4. Importantly, our data suggests day 11 CL acquire mechanisms to prevent blood vessel sprouting and promote their maturation by expressing NOTCH4 and JAG1, greatly enriched in luteal endothelial cells. Another endothelial specific gene, CD300LG, was identified here in the CL for the first time. CD300LG is an adhesion molecule enabling lymphocyte migration, its higher levels at mid cycle are expected to support the transmigration of immune cells into the CL at this stage. Together with steroidogenic genes, most of the genes regulating de-novo cholesterol biosynthetic pathway (e.g HMGCS, HMGCR) and cholesterol uptake from plasma (LDLR, APOD and APOE) were upregulated in the mature CL. These findings provide new insight of the processes involved in CL maturation including blood vessel growth and stabilization, leucocyte transmigration as well as progesterone synthesis as the CL matures.

Highlights

  • The ovulatory surge of gonadotropins triggers extensive structural, cellular, and molecular changes in the preovulatory follicle, leading to ovulation and corpus luteum (CL) formation [1, 2]

  • On day 4, the cluster enriched at the highest significance level, including 38 genes (>10% of the tested genes), was cell cycle (GO: 0007049) with a p-value of 3.10 e-20

  • Other selected clusters that were significantly enriched in day 4 CL data were: chromosome (GO: 0005694), DNA metabolic process (GO: 0006259), nucleoside binding (GO: 0001882) and DNA replication (GO: 0006260)

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Summary

Introduction

The ovulatory surge of gonadotropins triggers extensive structural, cellular, and molecular changes in the preovulatory follicle, leading to ovulation and corpus luteum (CL) formation [1, 2]. But is eventually composed of multiple, distinctive cell types including luteal steroidogenic cells (LSC; small and large cells that originate from theca and granulosa, respectively) and non-steroidogenic cells (luteal endothelial cells—LEC; pericytes, fibrocytes, and immune cells) [3,4,5,6]. Various immune cells such as lymphocytes, macrophages, neutrophils, eosinophils, and dendritic cells are identified in the mature CL [7,8,9,10,11]. The profile of select gene expression in these CL and in isolated luteal cell types (endothelial and steroidogenic) was validated with quantitative real-time PCR (qPCR)

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