Biosensor capability of the endometrium is mediated in part, by altered miRNA cargo from conceptus‐derived extracellular vesicles

Author:

De Bem Tiago H. C.12,Bridi Alessandra2,Tinning Haidee1,Sampaio Rafael Vilar2,Malo‐Estepa Irene1,Wang Dapeng34,Vasconcelos Elton J. R.3,Nociti Ricardo Perecin2,de Ávila Ana C. F. C. M.2,Rodrigues Sangalli Juliano2,Motta Igor Garcia5,Arantes Ataíde Jr Gilmar5,da Silva Júlio C. B.2,Fumie Watanabe Yeda6,Gonella‐Diaza Angela7,da Silveira Juliano C.2,Pugliesi Guilherme5,Vieira Meirelles Flávio2,Forde Niamh13

Affiliation:

1. Discovery and Translational Sciences Department, Leeds Institute of Cardiovascular and Metabolic Medicine, School of Medicine University of Leeds Leeds UK

2. Departamento de Medicina Veterinária, Faculdade de Zootecnia e Engenharia de Alimentos Universidade de São Paulo Pirassununga Brazil

3. LeedsOmics University of Leeds Leeds UK

4. National Heart and Lung Institute Imperial College London London UK

5. Department of Animal Reproduction, School of Veterinary Medicine and Animal Science University of São Paulo Pirassununga Brazil

6. Vitrogen – Biotecnologia em Reprodução Animal Cravinhos Brazil

7. North Florida Research and Education Center, Institute of Food and Agricultural Sciences University of Florida Gainesville Florida USA

Abstract

AbstractWe tested the hypothesis that the biosensor capability of the endometrium is mediated in part, by the effect of different cargo contained in the extracellular vesicles secreted by the conceptus during the peri‐implantation period of pregnancy. We transferred Bos taurus taurus embryos of different origin, in vivo (high developmental potential (IV)), in vitro (intermediate developmental potential (IVF)), or cloned (low developmental potential (NT)), into Bos taurus indicus recipients. Extracellular vesicles (EVs) recovered from Day 16 conceptus‐conditioned medium were characterized and their microRNA (miRNA) cargo sequenced alongside RNA sequencing of their respective endometria. There were substantial differences in the endometrial response to in vivo versus in vitro and in vivo versus cloned conceptuses (1153 and 334DEGs respectively) with limited differences between in vitro Vs cloned conceptuses (36 DEGs). The miRNA cargo contained in conceptus‐derived EVs was similar between all three groups (426 miRNA in common). Only 8 miRNAs were different between in vivo and cloned conceptuses, while only 6 miRNAs were different between in vivo and in vitro‐derived conceptuses. Treatment of endometrial epithelial cells with mimic or inhibitors for miR‐128 and miR‐1298 changed the proteomic content of target cells (96 and 85, respectively) of which mRNAs are altered in the endometrium in vivo (PLXDC2, COPG1, HSPA12A, MCM5, TBL1XR1, and TTF). In conclusion, we have determined that the biosensor capability of the endometrium is mediated in part, by its response to different EVs miRNA cargo produced by the conceptus during the peri‐implantation period of pregnancy.

Funder

Biotechnology and Biological Sciences Research Council

Fundação de Amparo à Pesquisa do Estado de São Paulo

Publisher

Wiley

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