Genetic lesions causing human male infertility are
manifold. Besides gross chromosomal aneuploidies and rearrangements, microdeletions and single gene defects
can interfere with male fertility.
Male
fertility is not only dependent on genes
controlling the male germ line but also on genes of the networks functional for
male gonad development and male somatic development, respectively. It is
popular to unravel these networks with mouse gene knock-out mutants displaying
reproductive defects. However, substantial arguments can be given for more
functional dies directly on the human genes, because multiple reproductive proteins evolve
quickly most likely for adopting to the specific needs of the species class.
Prominent examples are mutations of the FSHR gene causing different pathologies
in mouse and human and the DAZ gene family not found in the mouse genome but in the
human genome with an essential male fertility function. Therefore this review is focussed on a
comprehensive overview of human genes known with mutations causing male infertility
(AR; AZF gene families; CFTR, DM-1, DNAH gene family, FGFR1, FSHR, INSL3,KAL-1,
LGR8- GREAT, LHR, POLG).
Then some human genes are described well recognised
as functional in
spermatogenesis and male fertility although gene
specific mutations causing infertility were not yet identified (CREM,CDY1,
DAZL1, PHGPx, PRM-1, PRM-2). They are designated as “spermatogenesis phase
marker” or “male fertility
index” genes, because they are useful tools for
diagnosing the patient´s´ spermatogenesis disruption phase and for predicting
the presence and quality of his mature sperms. Current therapeutic protocols
for human male infertility do
usually not cure the specific gene defect but try to
bypass it using Artificial Reproductive Technology (ART). Putative imprinting
defects in the early embryo probably associated with the used ART protocol and
an increase of chromosome
abnormalities in the ART offspring now strongly asks
for a significant improvement of this outcome requesting urgently more basic
research on the genes functioning in the human male germ line and during early
human embryogenesis.
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