| Literature DB >> 33482360 |
Chunyu Huang1, Yong Zeng2, Wenwei Tu3.
Abstract
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Year: 2021 PMID: 33482360 PMCID: PMC8602393 DOI: 10.1016/j.gpb.2020.12.005
Source DB: PubMed Journal: Genomics Proteomics Bioinformatics ISSN: 1672-0229 Impact factor: 7.691
Figure 1Overactivation of immune status at maternal-fetal interface in RM/RPL patients
The proportion of pro-inflammatory immune cell subsets (e.g., dNK3, dM1, peripheral CD8+ effector T, MAIT, and CD56dimCD16+ NK cells) is increased, whereas the proportion of anti-inflammatory immune cell subsets (e.g., dNK1, dNK2, dM2, peripheral CD4+ naïve T, CD8+ naïve T, CD4+ memory T, and CD56brightCD16− NK cells) is decreased in decidua and peripheral blood, together leading to overactivation of immune status at the maternal-fetal interface in RM/RPL patients. dM, decidual macrophage; dNK, decidual NK; EVT, extravillous trophoblast; GPF, growth-promoting factor; MAIT, mucosal-associated invariant T; RM, recurrent miscarriage; RPL, recurrent pregnancy loss.