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Target Concepts:
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Query: UNIPROT:Q8IYM1 (
SEPT12
)
19
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The human septins are part of a gene family, that is a group of genes with similar sequences and usually but not invariably share similar functions that are descended from a common ancestor. Here we review our current knowledge of the human septin gene family and highlight areas of uncertainty. Currently 13 human septin genes are known (SEPT1 to
SEPT12
and SEPT14). What was known as SEPT13 is now defined as one of many
SEPT7
related pseudogenes. The family is characterized by complex genomics and extensive (but not universal) splicing, giving rise to a plethora of septin isoforms. For only a few members of the family do we have a comprehensive insight into these transcripts and isoforms. Given the formation of countless septin homotypic and heterotypic interactions our understanding of the biology and pathobiology of the septin family will require a detailed understanding of the genomics, transcriptomics and regulation of all members of this diverse and complex family.
...
PMID:Septin genomics: a road less travelled. 2180 95
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
Septins are GTP-binding and membrane-interacting proteins with a highly conserved domain structure involved in various cellular processes, including cytoskeleton organization, cytokinesis, and membrane dynamics. To date, 13 different septin genes have been identified in mammals (
SEPT1
to
SEPT12
and
SEPT14
), which can be classified into four distinct subgroups based on the sequence homology of their domain structure (SEPT2, SEPT3, SEPT6, and
SEPT7
subgroup). The family members of these subgroups have a strong affinity for other septins and form apolar tri-, hexa-, or octameric complexes consisting of multiple septin polypeptides. The first characterized core complex is the hetero-trimer SEPT2-6-7. Within these complexes single septins can be exchanged in a subgroup-specific manner. Hexamers contain SEPT2 and SEPT6 subgroup members and
SEPT7
in two copies each whereas the octamers additionally comprise two SEPT9 subgroup septins. The various isoforms seem to determine the function and regulation of the septin complex. Septins self-assemble into higher-order structures, including filaments and rings in orders, which are typical for different cell types. Misregulation of septins leads to human diseases such as neurodegenerative and bleeding disorders. In non-dividing cells such as neuronal tissue and platelets septins have been associated with exocytosis. However, many mechanistic details and roles attributed to septins are poorly understood. We describe here some important mammalian septin interactions with a special focus on the clinically relevant septin interactions.
...
PMID:The Mammalian Septin Interactome. 2822 24
Male infertility is observed in approximately 50% of all couples with infertility. Intracytoplasmic sperm injection (ICSI), a conventional artificial reproductive technique for treating male infertility, may fail because of a severe low sperm count, immotile sperm, immature sperm, and sperm with structural defects and DNA damage. Our previous studies have revealed that mutations in the septin (SEPT)-coding gene
SEPT12
cause teratozoospermia and severe oligozoospermia. These spermatozoa exhibit morphological defects in the head and tail, premature chromosomal condensation, and nuclear damage. Sperm from
Sept12
knockout mice also cause the developmental arrest of preimplantation embryos generated through in vitro fertilization and ICSI. Furthermore, we found that
SEPT12
interacts with SPAG4, a spermatid nuclear membrane protein that is also named SUN4. Loss of the
Spag4
allele in mice also disrupts the integration nuclear envelope and reveals sperm head defects. However, whether
SEPT12
affects SPAG4 during mammalian spermiogenesis remains unclear. We thus conducted this study to explore this question. First, we found that SPAG4 and
SEPT12
exhibited similar localizations in the postacrosomal region of elongating spermatids and at the neck of mature sperm through isolated murine male germ cells. Second,
SEPT12
expression altered the nuclear membrane localization of SPAG4, as observed through confocal microscopy, in a human testicular cancer cell line. Third,
SEPT12
expression also altered the localizations of nuclear membrane proteins: LAMINA/C in the cells. This effect was specifically due to the expression of
SEPT12
and not that of SEPT1, SEPT6,
SEPT7
, or SEPT11. Based on these results, we suggest that
SEPT12
is among the moderators of SPAG4/LAMIN complexes and is involved in the morphological formation of sperm during mammalian spermiogenesis.
...
PMID:Testis-Specific SEPT12 Expression Affects SUN Protein Localization and is Involved in Mammalian Spermiogenesis. 3086 52