Target Name: CLU
NCBI ID: G1191
Review Report on CLU Target / Biomarker Content of Review Report on CLU Target / Biomarker
CLU
Other Name(s): APO-J | ApoJalpha | Clusterin (CLU; Apo-J) | Complement cytolysis inhibitor | ApoJbeta | OTTHUMP00000225248 | Clusterin, transcript variant 1 | Aging-associated protein 4 | clusterin | epididymis secretory sperm binding protein | Testosterone-repressed prostate message 2 | Sulfated glycoprotein 2 | OTTHUMP00000225247 | APOJ | TRPM-2 | Apolipoprotein J | Complement-associated protein SP-40,40 | OTTHUMP00000225249 | ku70-binding protein 1 | CLU variant 1 | aging-associated protein 4 | Clusterin, transcript variant 3 | AAG4 | Aging-associated gene 4 protein | NA1/NA2 | Clusterin beta chain | Clusterin | MGC24903 | SGP-2 | CLU variant 3 | CLI | Complement cytolysis inhibitor b chain | Ku70-binding protein 1 | CLU2 | KUB1 | Complement cytolysis inhibitor a chain | sulfated glycoprotein 2 | Clusterin alpha chain | apolipoprotein J | CLUS_HUMAN | testosterone-repressed prostate message 2 | CLU1 | Complement lysis inhibitor | complement lysis inhibitor | complement-associated protein SP-40,40 | OTTHUMP00000128311 | SGP2 | complement cytolysis inhibitor | SP-40 | Apo-J | TRPM2

CLU: A Drug Target / Disease Biomarker

CLU is a protein that is expressed in various tissues throughout the body, including the brain, heart, kidneys, and intestines. It is a key regulator of cell division and has been implicated in a number of diseases, including cancer, neurodegenerative diseases, and autoimmune disorders.

Recent studies have identified CLU as a potential drug target for a variety of therapeutic approaches. One approach is to target CLU directly with small molecules, such as inhibitors or modulators, in order to reduce its activity and potentially disrupt its functions. Another approach is to target CLU through its downstream signaling pathways, such as the PI3K/Akt signaling pathway, in order to inhibit its activity and potentially lead to its degradation.

While more research is needed to fully understand the biology of CLU and its potential as a drug target, it is clear that CLU plays an important role in many diseases and is a promising target for future therapeutic interventions.

Protein Name: Clusterin

Functions: Functions as extracellular chaperone that prevents aggregation of non native proteins (PubMed:11123922, PubMed:19535339). Prevents stress-induced aggregation of blood plasma proteins (PubMed:11123922, PubMed:12176985, PubMed:17260971, PubMed:19996109). Inhibits formation of amyloid fibrils by APP, APOC2, B2M, CALCA, CSN3, SNCA and aggregation-prone LYZ variants (in vitro) (PubMed:12047389, PubMed:17412999, PubMed:17407782). Does not require ATP (PubMed:11123922). Maintains partially unfolded proteins in a state appropriate for subsequent refolding by other chaperones, such as HSPA8/HSC70 (PubMed:11123922). Does not refold proteins by itself (PubMed:11123922). Binding to cell surface receptors triggers internalization of the chaperone-client complex and subsequent lysosomal or proteasomal degradation (PubMed:21505792). Protects cells against apoptosis and against cytolysis by complement (PubMed:2780565). Intracellular forms interact with ubiquitin and SCF (SKP1-CUL1-F-box protein) E3 ubiquitin-protein ligase complexes and promote the ubiquitination and subsequent proteasomal degradation of target proteins (PubMed:20068069). Promotes proteasomal degradation of COMMD1 and IKBKB (PubMed:20068069). Modulates NF-kappa-B transcriptional activity (PubMed:12882985). A mitochondrial form suppresses BAX-dependent release of cytochrome c into the cytoplasm and inhibit apoptosis (PubMed:16113678, PubMed:17689225). Plays a role in the regulation of cell proliferation (PubMed:19137541). An intracellular form suppresses stress-induced apoptosis by stabilizing mitochondrial membrane integrity through interaction with HSPA5 (PubMed:22689054). Secreted form does not affect caspase or BAX-mediated intrinsic apoptosis and TNF-induced NF-kappa-B-activity (PubMed:24073260). Secreted form act as an important modulator during neuronal differentiation through interaction with STMN3 (By similarity). Plays a role in the clearance of immune complexes that arise during cell injury (By similarity)

The "CLU Target / Biomarker Review Report" is a customizable review of hundreds up to thousends of related scientific research literature by AI technology, covering specific information about CLU comprehensively, including but not limited to:
•   general information;
•   protein structure and compound binding;
•   protein biological mechanisms;
•   its importance;
•   the target screening and validation;
•   expression level;
•   disease relevance;
•   drug resistance;
•   related combination drugs;
•   pharmacochemistry experiments;
•   related patent analysis;
•   advantages and risks of development, etc.
The report is helpful for project application, drug molecule design, research progress updates, publication of research papers, patent applications, etc. If you are interested to get a full version of this report, please feel free to contact us at BD@silexon.ai

More Common Targets

CLUAP1 | CLUH | CLUHP3 | CLUHP8 | CLUL1 | CLVS1 | CLVS2 | CLXN | CLYBL | CLYBL-AS1 | CLYBL-AS2 | CLYBL-AS3 | CMA1 | CMAHP | CMAS | CMBL | CMC1 | CMC2 | CMC4 | CMG Helicase Complex | CMIP | CMKLR1 | CMKLR2 | CMKLR2-AS | CMPK1 | CMPK2 | CMSS1 | CMTM1 | CMTM2 | CMTM3 | CMTM4 | CMTM5 | CMTM6 | CMTM7 | CMTM8 | CMTR1 | CMTR2 | CMYA5 | CNBD1 | CNBD2 | CNBP | CNDP1 | CNDP2 | CNE9 | CNEP1R1 | CNFN | CNGA1 | CNGA2 | CNGA3 | CNGA4 | CNGB1 | CNGB3 | CNIH2 | CNIH3 | CNIH4 | CNKSR1 | CNKSR2 | CNKSR3 | CNMD | CNN1 | CNN2 | CNN2P2 | CNN2P4 | CNN3 | CNN3-DT | CNNM1 | CNNM2 | CNNM3 | CNNM4 | CNOT1 | CNOT10 | CNOT11 | CNOT2 | CNOT3 | CNOT4 | CNOT4P1 | CNOT6 | CNOT6L | CNOT6LP1 | CNOT7 | CNOT8 | CNOT9 | CNP | CNPPD1 | CNPY1 | CNPY2 | CNPY3 | CNPY4 | CNR1 | CNR2 | CNRIP1 | CNST | CNTD1 | CNTF | CNTFR | CNTLN | CNTN1 | CNTN2 | CNTN3 | CNTN4