Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
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Drug
Enzyme
Compound
Query: EC:3.4.22.54 (
calpain 3
)
430
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
In the course of cDNA cloning of the large subunits of human mu- and mCANPs, a novel cDNA clone encoding a putative calcium-dependent cysteine protease homologous to but distinct from both mu- and m-types was found. The encoded protein, designated tentatively as
p94
, is composed of four domains similar to those found in other
CANP
large subunits, but includes three unique regions that have no homology to other CANPs. These unique sequences might be involved in regulating the activation and/or determining the intracellular localization of
p94
. Since the mRNA for
p94
is five times more abundant than that for the CANP small subunit in skeletal muscle, it is possible that
p94
does not associate with the small subunit in vivo. In contrast to the ubiquitous expression of mu- and m-types, the mRNA for
p94
is expressed only in skeletal muscle. Besides acting as a protease,
p94
may act as a skeletal muscle specific regulatory protein like troponin C.
...
PMID:A novel member of the calcium-dependent cysteine protease family. 240 May 79
Two types of calcium-dependent protease with distinct calcium requirements (termed muCANP and mCANP) are known in mammalian tissues. These two isozymes consist of different large (80-kDa) subunits (mu- or m-types) and identical small (30-kDa) subunits. By screening human and rat muscle cDNA libraries with a cDNA probe for the chicken
CANP
large subunit, which has a structure similar to both the mammalian mu- and m-types, a cDNA clone encoding a novel member of the
CANP
large subunit family was obtained. The encoded protein (designated "p94") consists of 821 amino acid residues (Mr 94,084) and shows significant sequence homology with both human mu-type (54%) and m-type (51%) large subunits.
p94
can be divided into four domains (I-IV) as reported for the
CANP
large subunit family. Domains II and IV are potential cysteine protease and calcium-binding domains, respectively, and have sequences homologous to the corresponding domains of other
CANP
large subunits. However, domain I of
p94
is significantly different from others. Moreover,
p94
contains two unique sequences of 62 and 77 residues in domains II and III, respectively. In contrast to the ubiquitous expression of mu- and m-types, Northern blot analysis revealed that the mRNA for
p94
exists only in skeletal muscle with none detected in other tissues including heart muscle and smooth muscles such as intestine.
...
PMID:Molecular cloning of a novel mammalian calcium-dependent protease distinct from both m- and mu-types. Specific expression of the mRNA in skeletal muscle. 255 41
