ADAM10 is involved in cell junction assembly in early porcine embryo development

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Abstract

ADAM10 (A Disintegrin and Metalloprotease domain-containing protein 10) is a cell surface protein with a unique structure possessing both potential adhesion and protease domains. However, the role of ADAM10 in preimplantation stage embryos is not clear. In this study, we examined the expression patterns and functional roles of ADAM10 in porcine parthenotes during preimplantation development. The transcription level of ADAM10 dramatically increased from the morula stage onward. Immunostaining revealed that ADAM10 was present in both the nucleus and cytoplasm in early cleavage stage embryos, and localized to the apical region of the outer cells in morula and blastocyst embryos. Knockdown (KD) of ADAM10 using double strand RNA did not alter preimplantation embryo development until morula stage, but resulted in significantly reduced development to blastocyst stage. Moreover, the KD blastocyst showed a decrease in gene expression of adherens and tight junction (AJ/TJ), and an increase in trophectoderm TJ permeability by disrupting TJ assembly. Treatment with an ADAM10 specific chemical inhibitor, GI254023X, at the morula stage also inhibited blastocyst development and led to disruption of TJ assembly. An in situ proximity ligation assay demonstrated direct interaction of ADAM10 with coxsackie virus and adenovirus receptor (CXADR), supporting the involvement of ADAM10 in TJ assembly. In conclusion, our findings strongly suggest that ADADM10 is important for blastocyst formation rather than compaction, particularly for TJ assembly and stabilization in preimplantation porcine parthenogenetic development.

Figures

  • Fig 2. Knock-down (KD) of ADAM10 during early embryonic development. (A) KD efficiency of ADAM10 in blastocysts by qRT-PCR. (B) KD efficiency of ADAM10 in blastocysts by ICC. (C) Developmental competence of both control and knock-down groups. (D) Representative images of control and ADAM10 KD blastocysts at 144 h.p.a. Asterisks indicate statistically significant differences (P < 0.05). The data are presented as mean ± SEM. RQ: relative quantification; Scale bars: 200 μm.
  • Fig 5. Proximity ligation assay (PLA) in blastocysts and hypothetical model for the roles of ADAM10 in embryo development. ADAM10 and CXADR interaction in porcine blastocyst using PLA. Control: 144 h. p.a in PZM-5 (non-treatment); ADAM10 dsRNA: ADAM10 dsRNA injection after 8 h.p.a and culturing for 136 h; GI254023X (100 μM): GI254023X treatment after 96 h.p.a to 144 h.p.a.
  • Fig 6. A model of ADAM10 during blastocyst formation. The SH3 domains of CXADR and TJP1 interact with SH2 binding motif of the cytoplasmic domain of ADAM10. Tetraspanin proteins such as OCLN interact with the extracellular domains of ADAM10 or with TJP1, suggesting that the clustering of AJ and TJ mediated by ADAM10 provides strong TJ assembly and paracellular sealing, and leads to cavitation and expansion from the transition stage between morula and blastocyst and onwards.

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APA

Kwon, J., Jeong, S. M., Choi, I., & Kim, N. H. (2016). ADAM10 is involved in cell junction assembly in early porcine embryo development. PLoS ONE, 11(4). https://doi.org/10.1371/journal.pone.0152921

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