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Abstract
The new peptide hormone INSL3 is a member of the
insulin-relaxin family, yet unlike
insulin signals through a new G-protein coupled receptor,
LGR8, distantly related to the
receptors for LH and FSH. INSL3 is produced in large
amounts by the Leydig cells of
the testis in both fetal and adult mammals. Using a
combination of mRNA analysis by
reverse transcription polymerase chain reaction,
immunohistochemistry, ligand-binding,
and/or bioactivity assays, the distribution of LGR8
expression was assessed in
testicular tissues and cells, and in the epididymis. There
was consistent agreement that
LGR8 was expressed in meiotic and particularly postmeiotic
germ cells, and in Leydig
cells, though not in Sertoli or peritubular cells. Leydig
cells appear to express only a low
level of the LGR8 gene product; other transcripts may be
present, representing non-
functional products. mRNA analysis suggested that LGR8
transcripts in germ cells
represented mostly full-length forms. LGR8 mRNA was also
expressed in the
epididymis, though no function can yet be ascribed to this
expression. Therefore, the
INSL3/LGR8 system represents a further paracrine
hormone-receptor system in the
testis, which conveys information about Leydig cell status
to germ cells, and possibly as
part of an autocrine feedback loop.
Key words:
Testis •
Leydig cells •
Relaxin •
Spermatogenesis
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