Abstract

Testicular Sertoli cells phagocytose apoptotic spermatogenic cells in a manner depending on the membrane phospholipid phosphatidylserine (PS) expressed at the surface of the latter cell type. Our previous studies have indicated that class B scavenger receptor type I (SR-BI) is responsible for the PS-mediated phagocytosis by Sertoli cells. We examined here whether SR-BI binds directly to PS. A cell line acquired the ability to bind to PS-exposing apoptotic cells and to incorporate PS-containing liposomes when it was forced to express SR-BI. Furthermore, the extracellular domain of rat SR-BI fused with human Fc (SRBIecd-Fc) bound to PS with a dissociation equilibrium constant of 2.4 x 10(-7) m in a cell-free solid-phase assay, whereas other phospholipids including phosphatidylethanolamine, phosphatidylinositol, and phosphatidylcholine were poor binding targets. The binding activity was enhanced when CaCl(2) was included in the assay or when SRBIecd-Fc was pre-treated with N-glycanase. A portion of the extracellular domain spanning amino acid positions 33 and 191 (numbered with respect to the amino terminus) fused with Fc (SRBI33-191-Fc) showed activity and phospholipid specificity equivalent to those of SRBIecd-Fc. Finally, SRBI33-191-Fc bound to the surface of apoptotic cells with externalized PS, and the injection of SRBI33-191-Fc into the seminiferous tubules of live mice increased the number of apoptotic spermatogenic cells. These results allowed us to conclude that SR-BI is a phagocytosis-inducing PS receptor of Sertoli cells.

Highlights

  • During mammalian spermatogenic differentiation, more than half of the differentiating spermatogenic cells die, probably by apoptosis, before they mature into spermatozoa, the mechanism and functional significance of this phenomenon are unknown

  • We previously showed that rat Sertoli cells in primary cultures phagocytose apoptotic spermatogenic cells in a manner dependent on the membrane phospholipid phosphatidylserine (PS)1 exposed on the surface of the apoptotic cells and class B scavenger receptor type I (SR-BI) present in Sertoli cells [17,18,19]

  • PS-mediated Binding of Rat SR-BI-expressing Cells to Apoptotic Cells—In a previous study, we showed that Sertoli cellderived cell lines showed increased activity of both incorporating PS liposomes and phagocytosing apoptotic spermatogenic cells when they were transfected with rat SR-BI cDNA [19]

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Summary

Introduction

More than half of the differentiating spermatogenic cells die, probably by apoptosis, before they mature into spermatozoa (for review, see Refs. 1– 6), the mechanism and functional significance of this phenomenon are unknown. Our previous studies have indicated that class B scavenger receptor type I (SR-BI) is responsible for the PS-mediated phagocytosis by Sertoli cells.

Results
Conclusion
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