4.4 Article

Comparative proteome profiling of seminal components reveal impaired immune cell signalling as paternal contributors in recurrent pregnancy loss patients

Journal

Publisher

WILEY
DOI: 10.1111/aji.13613

Keywords

extracellular vesicle free seminal plasma; immune signalling; proteomics; recurrent pregnancy loss; seminal extracellular vesicles; spermatozoa

Ask authors/readers for more resources

Recent evidence suggests that male factors may be involved in recurrent pregnancy loss (RPL), as paternally expressed genes are predominant in the placenta. In this study, proteome profiling was carried out on seminal extracellular vesicles (SEVs), extracellular vesicle free seminal plasma (EVF-SP), and spermatozoa from RPL patients and fertile donors. The differentially expressed proteins in these samples were found to be associated with inflammatory response, immune cell signaling, and apoptosis. This suggests that altered cytokine levels in seminal components may contribute to impaired immune response and improper placental development in RPL.
Problem Recurrent pregnancy loss (RPL) is usually evaluated from a women's perspective, however, recent evidence implies involvement of male factors as paternally expressed genes predominate placenta. During fertilization, prior to implantation the immune system purposefully produces early pregnancy factors with potent immunomodulatory properties for adaptation to antigenically dissimilar embryo. Therefore, it is hypothesized that paternal immunological factors play a role in RPL. Method of study Comparative proteome profiling (label free liquid chromatography mass spectroscopy: LC-MS/MS) of the seminal extracellular vesicles (SEVs), extracellular vesicle free seminal plasma (EVF-SP) and spermatozoa was carried out in semen of RPL patients (n = 21) and fertile donors (n = 21). This was followed by pathway and protein-protein interaction analysis, and validation of key proteins' expression (western blot). Results A total of 68, 28 and 49 differentially expressed proteins in SEVs, EVF-SP and spermatozoa of RPL patients, respectively, were found to be involved in inflammatory response, immune cell signalling and apoptosis. In SEVs, underexpressed GDF-15 and overexpressed C3 imply distorted maternal immune response to paternal antigens leading to impaired decidualization. Dysregulated TGF beta signalling in EVF-SP surmises defective modulation of inflammatory response and induction of immune tolerance to seminal antigens in the female reproductive tract through generation of regulatory T cells. Retained histone variants in spermatozoa construe defective expression of early paternal genes, while underexpressed PTN may inflict defective angiogenesis resulting in expulsion of decidua. Conclusions Impaired modulation of immune response and improper placental development due to altered cytokine levels in seminal components may be the contributing paternal factors in RPL.

Authors

I am an author on this paper
Click your name to claim this paper and add it to your profile.

Reviews

Primary Rating

4.4
Not enough ratings

Secondary Ratings

Novelty
-
Significance
-
Scientific rigor
-
Rate this paper

Recommended

No Data Available
No Data Available