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Development of Recombinant PLC-Zeta Protein As a Therapeutic Intervention for the Clinical Treatment of Oocyte Activation Failure

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Journal Biomedicines
Date 2024 Jun 27
PMID 38927390
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Abstract

The sperm-specific phospholipase C zeta (PLCζ) protein is widely considered as the predominant physiological stimulus for initiating the Ca release responsible for oocyte activation during mammalian fertilization. The increasing number of genetic and clinical reports that directly link PLCζ defects and/or deficiencies with oocyte activation failure (OAF) necessitates the use of a powerful therapeutic intervention to overcome such cases of male factor infertility. Currently, in vitro fertilization (IVF) clinics treat OAF cases after intracytoplasmic sperm injection (ICSI) with Ca ionophores. Despite their successful use, such chemical agents are unable to trigger the physiological pattern of Ca oscillations. Moreover, the safety of these ionophores is not yet fully established. We have previously demonstrated that recombinant PLCζ protein can be successfully used to rescue failed oocyte activation, resulting in efficient blastocyst formation. Herein, we produced a maltose binding protein (MBP)-tagged recombinant human PLCζ protein capable of inducing Ca oscillations in mouse oocytes similar to those observed at fertilization. Circular dichroism (CD) experiments revealed a stable, well-folded protein with a high helical content. Moreover, the recombinant protein could retain its enzymatic properties for at least up to 90 days after storage at -80 °C. Finally, a chick embryo model was employed and revealed that exposure of fertilized chicken eggs to MBP-PLCζ did not alter the embryonic viability when compared to the control, giving a first indication of its safety. Our data support the potential use of the MBP-PLCζ recombinant protein as an effective therapeutic tool but further studies are required prior to its use in a clinical setting.

Citing Articles

Calcium signaling in oocyte quality and functionality and its application.

Chen C, Huang Z, Dong S, Ding M, Li J, Wang M Front Endocrinol (Lausanne). 2024; 15:1411000.

PMID: 39220364 PMC: 11361953. DOI: 10.3389/fendo.2024.1411000.

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