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• W2810370891 abstract "Does cellular composition of the endometrial biopsy affect the gene expression profile of endometrial whole-tissue samples? The differences in epithelial and stromal cell proportions in endometrial biopsies modify the whole-tissue gene expression profiles and affect the results of differential expression analyses. Each cell type has its unique gene expression profile. The proportions of epithelial and stromal cells vary in endometrial tissue during the menstrual cycle, along with individual and technical variation due to the method and tools used to obtain the tissue biopsy. Using cell-population specific transcriptome data and computational deconvolution approach, we estimated the epithelial and stromal cell proportions in whole-tissue biopsies taken during early secretory and mid-secretory phases. The estimated cellular proportions were used as covariates in whole-tissue differential gene expression analysis. Endometrial transcriptomes before and after deconvolution were compared and analysed in biological context. Paired early- and mid-secretory endometrial biopsies were obtained from 35 healthy, regularly cycling, fertile volunteers, aged 23–36 years, and analysed by RNA sequencing. Differential gene expression analysis was performed using two approaches. In one of them, computational deconvolution was applied as an intermediate step to adjust for the proportions of epithelial and stromal cells in the endometrial biopsy. The results were then compared to conventional differential expression analysis. Ten paired endometrial samples were analysed with qPCR to validate the results. The estimated average proportions of stromal and epithelial cells in early secretory phase were 65% and 35%, and during mid-secretory phase, 46% and 54%, respectively, correlating well with the results of histological evaluation (r = 0.88, P = 1.1 × 10−6). Endometrial tissue transcriptomic analysis showed that approximately 26% of transcripts (n = 946) differentially expressed in receptive endometrium in cell-type unadjusted analysis also remain differentially expressed after adjustment for biopsy cellular composition. However, the other 74% (n = 2645) become statistically non-significant after adjustment for biopsy cellular composition, underlining the impact of tissue heterogeneity on differential expression analysis. The results suggest new mechanisms involved in endometrial maturation, involving genes like LINC01320, SLC8A1 and GGTA1P, described for the first time in context of endometrial receptivity. The RNA-seq data presented in this study is deposited in the Gene Expression Omnibus database with accession number GSE98386. Only dominant endometrial cell types were considered in gene expression profile deconvolution; however, other less frequent endometrial cell types also contribute to the whole-tissue gene expression profile. The better understanding of molecular processes during transition from pre-receptive to receptive endometrium serves to improve the effectiveness and personalization of assisted reproduction protocols. Biopsy cellular composition should be taken into account in future endometrial ‘omics’ studies, where tissue heterogeneity could potentially influence the results. This study was funded by: Estonian Ministry of Education and Research (grant IUT34-16); Enterprise Estonia (EU48695); the EU-FP7 Eurostars program (NOTED, EU41564); the EU-FP7 Marie Curie Industry-Academia Partnerships and Pathways (SARM, EU324509); Horizon 2020 innovation program (WIDENLIFE, EU692065); MSCA-RISE-2015 project MOMENDO (No 691058) and the Miguel Servet Program Type I of Instituto de Salud Carlos III (CP13/00038); Spanish Ministry of Economy, Industry and Competitiveness (MINECO) and European Regional Development Fund (FEDER): grants RYC-2016-21199 and ENDORE SAF2017-87526. Authors confirm no competing interests." @default.
• W2810370891 created "2018-07-10" @default.
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• W2810370891 date "2018-10-08" @default.
• W2810370891 modified "2023-10-09" @default.
• W2810370891 title "Endometrial receptivity revisited: endometrial transcriptome adjusted for tissue cellular heterogeneity" @default.
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• W2810370891 cites W1985987855 @default.
• W2810370891 cites W1995706668 @default.
• W2810370891 cites W2003778314 @default.
• W2810370891 cites W2031502301 @default.
• W2810370891 cites W2035693178 @default.
• W2810370891 cites W2048354906 @default.
• W2810370891 cites W2053266958 @default.
• W2810370891 cites W2057427640 @default.
• W2810370891 cites W2065912007 @default.
• W2810370891 cites W2069902854 @default.
• W2810370891 cites W2070421129 @default.
• W2810370891 cites W2083888181 @default.
• W2810370891 cites W2084150775 @default.
• W2810370891 cites W2084669890 @default.
• W2810370891 cites W2095082636 @default.
• W2810370891 cites W2095346603 @default.
• W2810370891 cites W2107277218 @default.
• W2810370891 cites W2109820937 @default.
• W2810370891 cites W2114104545 @default.
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• W2810370891 cites W2123982689 @default.
• W2810370891 cites W2124156734 @default.
• W2810370891 cites W2127368795 @default.
• W2810370891 cites W2129375421 @default.
• W2810370891 cites W2131993172 @default.
• W2810370891 cites W2133520037 @default.
• W2810370891 cites W2134526812 @default.
• W2810370891 cites W2143390537 @default.
• W2810370891 cites W2143750395 @default.
• W2810370891 cites W2153290165 @default.
• W2810370891 cites W2156292936 @default.
• W2810370891 cites W2158549544 @default.
• W2810370891 cites W2158906685 @default.
• W2810370891 cites W2160327376 @default.
• W2810370891 cites W2162143298 @default.
• W2810370891 cites W2164002837 @default.
• W2810370891 cites W2166681530 @default.
• W2810370891 cites W2167896519 @default.
• W2810370891 cites W2204640292 @default.
• W2810370891 cites W2301339423 @default.
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• W2810370891 cites W2605502123 @default.
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• W2810370891 doi "https://doi.org/10.1093/humrep/dey301" @default.
• W2810370891 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30295736" @default.
• W2810370891 hasPublicationYear "2018" @default.
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