Analysis of weighted gene co-expression networks and clinical validation identify hub genes and immune cell infiltration in the endometrial cells of patients with recurrent implantation failure
Zhenteng Liu, Shoucui Lai, Qinglan Qu, Xuemei Liu, Wei Zhang, Dongmei Zhao, Shunzhi He, Yuxia Sun, Hongchu Bao

TL;DR
This study identifies key genes and immune cell changes in the endometrium of patients with recurrent implantation failure, offering new insights into its genetic and immune causes.
Contribution
The first use of WGCNA to identify nine hub genes linked to RIF and the analysis of immune infiltration patterns in RIF endometrium.
Findings
Nine hub genes (ACTL6A, BECN1, SNRPD1, etc.) were identified as potentially involved in RIF.
Immune infiltration patterns showed altered uNK and CD4+ T cells in RIF endometrium.
Genes may contribute to RIF by disrupting endometrial microflora, autophagy, and cell proliferation.
Abstract
About 10% of individuals undergoing in vitro fertilization encounter recurrent implantation failure (RIF), which represents a worldwide social and economic concern. Nevertheless, the critical genes and genetic mechanisms underlying RIF are largely unknown. We first obtained three comprehensive microarray datasets “GSE58144, GSE103465 and GSE111974”. The differentially expressed genes (DEGs) evaluation, enrichment analysis, as well as efficient weighted gene co-expression network analysis (WGCNA), were employed for distinguishing RIF-linked hub genes, which were tested by RT-qPCR in our 30 independent samples. Next, we studied the topography of infiltration of 22 immune cell subpopulations and the association between hub genes and immune cells in RIF using the CIBERSORT algorithm. Finally, a novel ridge plot was utilized to exhibit the potential function of core genes. The enrichment…
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Taxonomy
TopicsReproductive System and Pregnancy · Endometriosis Research and Treatment · Reproductive Physiology in Livestock
