Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UNIPROT:Q8IYM1 (
SEPT12
)
19
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Male infertility has become a worldwide health problem, but the etiologies of most cases are still unknown.
SEPT12
, a GTP-binding protein, is involved in male fertility. Two
SEPT12
mutations (
SEPT12
(T89M) and
SEPT12
(D197N)) have been identified in infertile men who have a defective sperm annulus with a bent tail. The function of
SEPT12
in the sperm annulus is still unclear. Here, we found that
SEPT12
formed a filamentous structure with SEPT7, SEPT 6, SEPT2 and
SEPT4
at the sperm annulus. The
SEPT12
-based septin core complex was assembled as octameric filaments comprising the SEPT proteins 12-7-6-2-2-6-7-12 or 12-7-6-4-4-6-7-12. In addition, the GTP-binding domain of
SEPT12
was crucial for its interaction with SEPT7, and the N- and C-termini of
SEPT12
were required for the interaction of
SEPT12
with itself to polymerize octamers into filaments. Mutant mice carrying the
SEPT12
(D197N) mutation, which disrupts
SEPT12
filament formation, showed a disorganized sperm annulus, bent tail, reduced motility and loss of the SEPT ring structure at the sperm annulus. These phenotypes were also observed in an infertile man carrying
SEPT12
(D197N). Taken together, our results demonstrate the molecular architecture of
SEPT12
filaments at the sperm annulus, their mechanical support of sperm motility, and their correlation with male infertility.
...
PMID:SEPT12 orchestrates the formation of mammalian sperm annulus by organizing core octameric complexes with other SEPT proteins. 2558 30
Male infertility affects approximately 50% of all infertile couples. The male-related causes of intracytoplasmic sperm injection failure include the absence of sperm, immotile or immature sperm, and sperm with structural defects such as those caused by premature chromosomal condensation and DNA damage. Our previous studies based on a knockout mice model indicated that
SEPT12
proteins are critical for the terminal morphological formation of sperm.
SEPT12
mutations in men result in teratozospermia and oligozospermia. In addition, the spermatozoa exhibit morphological defects of the head and tail, premature chromosomal condensation, and nuclear damage. However, the molecular functions of
SEPT12
during spermatogenesis remain unclear. To determine the molecular functions of
SEPT12
, we applied a yeast 2-hybrid system to identify
SEPT12
interactors. Seven proteins that interact with
SEPT12
were identified: SEPT family proteins (
SEPT4
and SEPT6), nuclear or nuclear membrane proteins (protamine 2, sperm-associated antigen 4, and NDC1 transmembrane nucleoproine), and sperm-related structural proteins (pericentriolar material 1 and obscurin-like 1). Sperm-associated antigen 4 (SPAG4; also known as SUN4) belongs to the SUN family of proteins and acts as a linker protein between nucleoskeleton and cytoskeleton proteins and localizes in the nuclear membrane. We determined that
SEPT12
interacts with SPAG4 in a male germ cell line through coimmunoprecipitation. During human spermiogenesis,
SEPT12
is colocalized with SPAG4 near the nuclear periphery in round spermatids and in the centrosome region in elongating spermatids. Furthermore, we observed that
SEPT12
/SPAG4/LAMINB1 formed complexes and were coexpressed in the nuclear periphery of round spermatids. In addition, mutated
SEPT12
, which was screened from an infertile man, affected the integration of these nuclear envelope complexes through coimmunoprecipitation. This was the first study that suggested that SEPT proteins link to the SUN/LAMIN complexes during the formation of nuclear envelopes and are involved in the development of postmeiotic germ cells.
...
PMID:SEPT12/SPAG4/LAMINB1 complexes are required for maintaining the integrity of the nuclear envelope in postmeiotic male germ cells. 2577 3
