4.4 Article

Soluble human leukocyte antigen-G is a potential embryo viability biomarker and a positive predictor of live-births in humans

Journal

Publisher

WILEY
DOI: 10.1111/aji.13499

Keywords

biomarker; embryo-viability; noninvasive; pregnancy outcome; sHLA-G

Funding

  1. IMPRINT program [4511]
  2. Ministry of Human Resource Development
  3. Indian Council of Medical Research (ICMR), Govt. of India
  4. DBT-IISc Partnership program [22-0307-0018-05-496]

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This study investigated the association of embryo-secreted soluble human leukocyte antigen-G (sHLA-G) with developing embryos and its ability to predict successful pregnancy outcome. The levels of sHLA-G varied within and across clinics and different stages of embryonic development. While there was no significant correlation between sHLA-G levels and embryo morphology scores, levels of sHLA-G were significantly higher in live-birth cases compared to no-birth cases, particularly in blastocysts-ETs. The results suggest that sHLA-G can be a valuable biomarker to predict live-birth outcome in assisted reproductive technology.
Problem Human infertility affects 15-20% of reproductive-age couples and it is mitigated by assisted reproductive technology (ART) approaches. Poor biological viability of embryos contributes to implantation failure and live birth rate (LBR). This study is aimed to examine whether or not embryo-secreted soluble human leukocyte antigen-G (sHLA-G) is (i) associated with developing embryos and (ii) able to predict successful pregnancy outcome. Method of study A retrospective, multicentric study using 539 human embryo spent medium samples (E-SMs), analysed for sHLA-G levels by ELISA. Correlation analysis was performed on sHLA-G levels with developing embryonic stages, their quality scores and pregnancy outcome in terms of LBR. Results Of 539 E-SMs analysed, 445 had detectable sHLA-G (83%) with levels varying within and across clinics and, between stages of embryonic development. Levels of sHLA-G (ng/mL) were significantly (P < .05) different in E-SMs of cleavage-stage embryos versus blastocysts. There was an insignificant correlation between the sHLA-G levels and morphology scores of embryos. But, sHLA-G levels showed a positive correlation with grades of blastocysts and importantly, its levels were significantly (P < .05) higher in live-birth vis-a-vis no-birth cases. Also, levels were higher in live-births out of blastocysts-ETs versus cleavage-stage-embryo transfers. Altered levels were observed with embryos, which resulted in miscarriages. Overall, a significant (P < .0001) association of sHLA-G with live births was observed. Conclusion Embryo-derived sHLA-G can be a valuable embryo viability, independent, biomarker, which can predict live-birth outcome and it could be useful as an adjunct to existing criteria for elective single embryo transfer.

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