ADAM10

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ADAM10 endopeptidase
ADAM10 endopeptidase
Identifiers
EC no.	3.4.24.81
CAS no.	193099-09-1
Databases
IntEnz	IntEnz view
BRENDA	BRENDA entry
ExPASy	NiceZyme view
KEGG	KEGG entry
MetaCyc	metabolic pathway
PRIAM	profile
PDB structures	RCSB PDB PDBe PDBsum
PMC
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PMC	articles
PubMed	articles
NCBI	proteins

ADAM10
Available structures
PDB	Ortholog search: PDBe RCSB
List of PDB id codes
	1M1I
Identifiers
Aliases	ADAM10, AD10, AD18, CD156c, HsT18717, MADM, RAK, kuz, CDw156, ADAM metallopeptidase domain 10
External IDs	OMIM: 602192 MGI: 109548 HomoloGene: 865 GeneCards: ADAM10
Gene location (Human)
Chr.	Chromosome 15 (human)
End	58,749,791 bp
Gene location (Mouse)
Chr.	Chromosome 9 (mouse)
End	70,687,511 bp
RNA expression pattern
	Top expressed in
	stromal cell of endometrium; ; amniotic fluid; ; visceral pleura; ; trigeminal ganglion; ; monocyte; ; oocyte; ; olfactory bulb; ; placenta; ; bone marrow cells; ; corpus callosum;
	Top expressed in
	cumulus cell; ; atrioventricular valve; ; atrium; ; mucous cell of stomach; ; molar; ; left lung lobe; ; urothelium; ; iris; ; conjunctival fornix; ; medullary collecting duct;
	More reference expression data
	; ; ; ;
	More reference expression data
Gene ontology
Molecular function	protein homodimerization activity; SH3 domain binding; endopeptidase activity; metal ion binding; integrin binding; peptidase activity; protein binding; signaling receptor binding; hydrolase activity; protein kinase binding; metallopeptidase activity; metalloendopeptidase activity;
Cellular component	cytoplasm; integral component of membrane; membrane; postsynaptic density; focal adhesion; plasma membrane; perinuclear endoplasmic reticulum; Golgi-associated vesicle; tetraspanin-enriched microdomain; extracellular exosome; nucleus; cell surface; Golgi membrane; extracellular space; Golgi apparatus; specific granule membrane; tertiary granule membrane; endoplasmic reticulum lumen; trans-Golgi network; synaptic vesicle; dendrite; neuronal cell body; dendritic spine; postsynaptic membrane; postsynapse; glutamatergic synapse;
Biological process	Notch signaling pathway; positive regulation of cell migration; ephrin receptor signaling pathway; cell-cell signaling; constitutive protein ectodomain proteolysis; protein processing; extracellular matrix disassembly; in utero embryonic development; proteolysis; monocyte activation; response to tumor necrosis factor; protein phosphorylation; positive regulation of cell growth; positive regulation of T cell chemotaxis; positive regulation of cell population proliferation; Notch receptor processing; integrin-mediated signaling pathway; membrane protein ectodomain proteolysis; negative regulation of cell adhesion; neutrophil degranulation; post-translational protein modification; spermatogenesis; amyloid-beta formation; Notch receptor processing, ligand-dependent; positive regulation of apoptotic process; regulation of dendritic spine morphogenesis; response to antineoplastic agent; regulation of neurotransmitter receptor localization to postsynaptic specialization membrane; postsynapse organization;
	Sources:Amigo / QuickGO
Orthologs
	102
	11487
	ENSG00000137845
	ENSMUSG00000054693
	O14672
	O35598
	NM_001110; NM_001320570
	NM_007399
	NP_001101; NP_001307499; NP_001101.1
	NP_031425
	Wikidata
View/Edit Human	View/Edit Mouse

A Disintegrin and metalloproteinase domain-containing protein 10, also known as ADAM10 or CDw156 or CD156c is a protein that in humans is encoded by the ADAM10 gene.^[5]

Function

Members of the ADAM family are cell surface proteins with a unique structure, possessing both potential adhesion and protease domains. Sheddase, a generic name for the ADAM metallopeptidase, functions primarily to cleave membrane proteins at the cellular surface. Once cleaved, the sheddases release soluble ectodomains with an altered location and function.^[6]^[7]^[8]

Although a single sheddase may “shed” a variety of substances, multiple sheddases can cleave the same substrate resulting in different consequences. This gene encodes an ADAM family member that cleaves many proteins including TNF-alpha and E-cadherin.^[5]

ADAM10 (EC#: 3.4.24.81) is a sheddase, and has a broad specificity for peptide hydrolysis reactions.^[9]

ADAM10 cleaves ephrin, within the ephrin/eph complex, formed between two cell surfaces. When ephrin is freed from the opposing cell, the entire ephrin/eph complex is endocytosed. This shedding in trans had not been previously shown, but may well be involved in other shedding events.^[10]

In neurons, ADAM10 is the most important enzyme, with α-secretase activity for proteolytic processing of the amyloid precursor protein.^[11] ADAM10, along with ADAM17, cleaves the ectodomain of the triggering receptor expressed on myeloid cells 2 (TREM2), to produce soluble TREM2 (sTREM2), which has been proposed as a CSF and sera biomarker of neurodegeneration.^[12]

ADAM10 belongs to subfamily A, the most ancestral subfamily of ADAM proteins, which is shared by all major groups of animals, choanoflagellates, fungi, and green algae from the class Mamiellophyceae.^[13]

Structure

Although no crystallographic x-ray diffraction analyses have been published that depict the entire structure of ADAM10, one domain has been studied using this technique. The disintegrin and cysteine-rich domain (shown to the right) plays an essential role in regulation of protease activity in vivo. Recent experimental evidence suggests that this region, which is distinct from the active site, may be responsible for substrate specificity of the enzyme. It is proposed that this domain binds to particular regions of the enzyme's substrate, allowing peptide bond hydrolysis to occur in well defined locations on certain substrate proteins.^[14]

The proposed active site of ADAM10 has been identified by sequence analysis, and is identical to enzymes in the Snake Venom metalloprotein domain family. The consensus sequence for catalytically active ADAM proteins is HEXGHNLGXXHD. Structural analysis of ADAM17, which has the same active site sequence as ADAM10, suggests that the three histidines in this sequence bind a Zn²⁺ atom, and that the glutamate is the catalytic residue.^[15]

Catalytic Mechanism

Although the exact mechanism of ADAM10 has not been thoroughly investigated, its active site is homologous to those of well studied zinc-proteases such as carboxypeptidase A and thermolysin. Therefore, it is proposed that ADAM10 utilizes a similar mechanism as these enzymes. In zinc proteases, the key catalytic elements have been identified as a glutamate residue and a Zn²⁺ ion coordinated to histidine residues.^[16]

The proposed mechanism begins with deprotonation of a water molecule by glutamate. The resultant hydroxide initiates a nucleophilic attack on a carbonyl carbon on the peptide backbone, producing a tetrahedral intermediate. This step is facilitated by electron withdrawal from oxygen by Zn²⁺ and by zinc's subsequent stabilization of the negative charge on the oxygen atom in the intermediate state. As electrons move down from the oxygen atom to re-form the double bond, the tetrahedral intermediate collapses to products with protonation of -NH by the glutamate residue.^[16]

Clinical significance

Brain diseases

ADAM10 plays a key role in the modulation of the molecular mechanisms responsible for dendritic spine formation, maturation and stabilization and in the regulation of the molecular organization of the glutamatergic synapse. Consequently, an alteration of ADAM10 activity is strictly correlated to the onset of different types of synaptopathies, ranging from neurodevelopmental disorders, i.e. autism spectrum disorders, to neurodegenerative diseases, i.e. Alzheimer's Disease.^[17]

Interaction with the malaria parasite

A number of different proteins on the surface of Plasmodium falciparum malaria parasites help the invaders bind to red blood cells. But once attached to host blood cells, the parasites need to shed the 'sticky' surface proteins that would otherwise interfere with entrance into the cell. The Sheddase enzyme, specifically called PfSUB2 in this example, is required for the parasites to invade cells; without it, the parasites die. The sheddase is stored in and released from cellular compartments near the tip of the parasite, according to the study. Once on the surface, the enzyme attaches to a motor that shuttles it from front to back, liberating the sticky surface proteins. With these proteins removed, the parasite gains entrance into a red blood cell. The entire invasion lasts about 30 seconds and without this ADAM metallopeptidase, malaria would be ineffective at invading the red blood cells.^[18]

Breast cancer

In combination with low doses of herceptin, selective ADAM10 inhibitors decrease proliferation in HER2 over-expressing cell lines while inhibitors, that do not inhibit ADAM10, have no impact. These results are consistent with ADAM10 being a major determinant of HER2 shedding, the inhibition of which, may provide a novel therapeutic approach for treating breast cancer and a variety of other cancers with active HER2 signaling.^[19]

The presence of the product of this gene in neuronal synapses in conjunction with protein AP2 has been seen in increased amounts in the hippocampal neurons of Alzheimer's disease patients.^[20]

References

^ ^a ^b ^c GRCh38: Ensembl release 89: ENSG00000137845 – Ensembl, May 2017
^ ^a ^b ^c GRCm38: Ensembl release 89: ENSMUSG00000054693 – Ensembl, May 2017
^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
^ ^a ^b "Entrez Gene: ADAM10 ADAM metallopeptidase domain 10".
^ Moss ML, Bartsch JW (June 2004). "Therapeutic benefits from targeting of ADAM family members". Biochemistry. 43 (23): 7227–35. doi:10.1021/bi049677f. PMID 15182168.
^ Nagano O, Saya H (December 2004). "Mechanism and biological significance of CD44 cleavage". Cancer Science. 95 (12): 930–5. doi:10.1111/j.1349-7006.2004.tb03179.x. PMID 15596040. S2CID 9009213.
^ Blobel CP (January 2005). "ADAMs: key components in EGFR signalling and development". Nature Reviews. Molecular Cell Biology. 6 (1): 32–43. doi:10.1038/nrm1548. PMID 15688065. S2CID 7011302.
^ "Entry of ADAM10 endopeptidase (EC-Number 3.4.24.81 )".
^ Janes PW, Saha N, Barton WA, Kolev MV, Wimmer-Kleikamp SH, Nievergall E, et al. (October 2005). "Adam meets Eph: an ADAM substrate recognition module acts as a molecular switch for ephrin cleavage in trans". Cell. 123 (2): 291–304. doi:10.1016/j.cell.2005.08.014. PMID 16239146. S2CID 7962666.
^ Haass C, Kaether C, Thinakaran G, Sisodia S (May 2012). "Trafficking and proteolytic processing of APP". Cold Spring Harbor Perspectives in Medicine. 2 (5): a006270. doi:10.1101/cshperspect.a006270. PMC 3331683. PMID 22553493.
^ Yang J, Fu Z, Zhang X, Xiong M, Meng L, Zhang Z (2020-07-07). "TREM2 ectodomain and its soluble form in Alzheimer's disease". Journal of Neuroinflammation. 17 (1): 204. doi:10.1186/s12974-020-01878-2. ISSN 1742-2094. PMC 7341574. PMID 32635934.
^ Souza J, Lisboa A, Santos T, Andrade M, Neves V, Teles-Souza J, et al. (2020). "The evolution of ADAM gene family in eukaryotes". Genomics. 112 (5): 3108–3116. doi:10.1016/j.ygeno.2020.05.010. PMID 32437852. S2CID 218832838.
^ Smith KM, Gaultier A, Cousin H, Alfandari D, White JM, DeSimone DW (December 2002). "The cysteine-rich domain regulates ADAM protease function in vivo". The Journal of Cell Biology. 159 (5): 893–902. doi:10.1083/jcb.200206023. PMC 2173380. PMID 12460986.
^ Wolfsberg TG, Primakoff P, Myles DG, White JM (October 1995). "ADAM, a novel family of membrane proteins containing A Disintegrin And Metalloprotease domain: multipotential functions in cell-cell and cell-matrix interactions". The Journal of Cell Biology. 131 (2): 275–8. doi:10.1083/jcb.131.2.275. PMC 2199973. PMID 7593158.
^ ^a ^b Lolis E, Petsko GA (1990). "Transition-state analogues in protein crystallography: probes of the structural source of enzyme catalysis". Annual Review of Biochemistry. 59: 597–630. doi:10.1146/annurev.bi.59.070190.003121. PMID 2197984.
^ Marcello E, Borroni B, Pelucchi S, Gardoni F, Di Luca M (November 2017). "ADAM10 as a therapeutic target for brain diseases: from developmental disorders to Alzheimer's disease". Expert Opinion on Therapeutic Targets. 21 (11): 1017–1026. doi:10.1080/14728222.2017.1386176. PMID 28960088. S2CID 46800368.
^ "'Sheddase' helps the malaria parasite invade red blood cells". Archived from the original on 2008-04-12.
^ Liu PC, Liu X, Li Y, Covington M, Wynn R, Huber R, et al. (June 2006). "Identification of ADAM10 as a major source of HER2 ectodomain sheddase activity in HER2 overexpressing breast cancer cells". Cancer Biology & Therapy. 5 (6): 657–64. doi:10.4161/cbt.5.6.2708. PMID 16627989. S2CID 23463401.
^ Marcello E, Saraceno C, Musardo S, Vara H, de la Fuente AG, Pelucchi S, et al. (June 2013). "Endocytosis of synaptic ADAM10 in neuronal plasticity and Alzheimer's disease". The Journal of Clinical Investigation. 123 (6): 2523–38. doi:10.1172/JCI65401. PMC 3668814. PMID 23676497.

External links

ADAM10 human gene location in the UCSC Genome Browser.
ADAM10 human gene details in the UCSC Genome Browser.
Overview of all the structural information available in the PDB for UniProt: O14672 (Disintegrin and metalloproteinase domain-containing protein 10) at the PDBe-KB.

This article incorporates text from the United States National Library of Medicine, which is in the public domain.

[refGRCh38Ensembl-1] GRCh38: Ensembl release 89: ENSG00000137845 – Ensembl, May 2017

[refGRCm38Ensembl-2] GRCm38: Ensembl release 89: ENSMUSG00000054693 – Ensembl, May 2017

[3] "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.

[4] "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.

[entrez-5] "Entrez Gene: ADAM10 ADAM metallopeptidase domain 10".

[pmid15182168-6] Moss ML, Bartsch JW (June 2004). "Therapeutic benefits from targeting of ADAM family members". Biochemistry. 43 (23): 7227–35. doi:10.1021/bi049677f. PMID 15182168.

[pmid15596040-7] Nagano O, Saya H (December 2004). "Mechanism and biological significance of CD44 cleavage". Cancer Science. 95 (12): 930–5. doi:10.1111/j.1349-7006.2004.tb03179.x. PMID 15596040. S2CID 9009213.

[pmid15688065-8] Blobel CP (January 2005). "ADAMs: key components in EGFR signalling and development". Nature Reviews. Molecular Cell Biology. 6 (1): 32–43. doi:10.1038/nrm1548. PMID 15688065. S2CID 7011302.

[Brenda_Database-9] "Entry of ADAM10 endopeptidase (EC-Number 3.4.24.81 )".

[pmid16239146-10] Janes PW, Saha N, Barton WA, Kolev MV, Wimmer-Kleikamp SH, Nievergall E, et al. (October 2005). "Adam meets Eph: an ADAM substrate recognition module acts as a molecular switch for ephrin cleavage in trans". Cell. 123 (2): 291–304. doi:10.1016/j.cell.2005.08.014. PMID 16239146. S2CID 7962666.

[11] Haass C, Kaether C, Thinakaran G, Sisodia S (May 2012). "Trafficking and proteolytic processing of APP". Cold Spring Harbor Perspectives in Medicine. 2 (5): a006270. doi:10.1101/cshperspect.a006270. PMC 3331683. PMID 22553493.

[12] Yang J, Fu Z, Zhang X, Xiong M, Meng L, Zhang Z (2020-07-07). "TREM2 ectodomain and its soluble form in Alzheimer's disease". Journal of Neuroinflammation. 17 (1): 204. doi:10.1186/s12974-020-01878-2. ISSN 1742-2094. PMC 7341574. PMID 32635934.

[ada-13] Souza J, Lisboa A, Santos T, Andrade M, Neves V, Teles-Souza J, et al. (2020). "The evolution of ADAM gene family in eukaryotes". Genomics. 112 (5): 3108–3116. doi:10.1016/j.ygeno.2020.05.010. PMID 32437852. S2CID 218832838.

[pmid12460986-14] Smith KM, Gaultier A, Cousin H, Alfandari D, White JM, DeSimone DW (December 2002). "The cysteine-rich domain regulates ADAM protease function in vivo". The Journal of Cell Biology. 159 (5): 893–902. doi:10.1083/jcb.200206023. PMC 2173380. PMID 12460986.

[pmid7593158-15] Wolfsberg TG, Primakoff P, Myles DG, White JM (October 1995). "ADAM, a novel family of membrane proteins containing A Disintegrin And Metalloprotease domain: multipotential functions in cell-cell and cell-matrix interactions". The Journal of Cell Biology. 131 (2): 275–8. doi:10.1083/jcb.131.2.275. PMC 2199973. PMID 7593158.

[pmid2197984-16] Lolis E, Petsko GA (1990). "Transition-state analogues in protein crystallography: probes of the structural source of enzyme catalysis". Annual Review of Biochemistry. 59: 597–630. doi:10.1146/annurev.bi.59.070190.003121. PMID 2197984.

[MarcelloBorroni2017-17] Marcello E, Borroni B, Pelucchi S, Gardoni F, Di Luca M (November 2017). "ADAM10 as a therapeutic target for brain diseases: from developmental disorders to Alzheimer's disease". Expert Opinion on Therapeutic Targets. 21 (11): 1017–1026. doi:10.1080/14728222.2017.1386176. PMID 28960088. S2CID 46800368.

[Malaria-18] "'Sheddase' helps the malaria parasite invade red blood cells". Archived from the original on 2008-04-12.

[pmid16627989-19] Liu PC, Liu X, Li Y, Covington M, Wynn R, Huber R, et al. (June 2006). "Identification of ADAM10 as a major source of HER2 ectodomain sheddase activity in HER2 overexpressing breast cancer cells". Cancer Biology & Therapy. 5 (6): 657–64. doi:10.4161/cbt.5.6.2708. PMID 16627989. S2CID 23463401.

[20] Marcello E, Saraceno C, Musardo S, Vara H, de la Fuente AG, Pelucchi S, et al. (June 2013). "Endocytosis of synaptic ADAM10 in neuronal plasticity and Alzheimer's disease". The Journal of Clinical Investigation. 123 (6): 2523–38. doi:10.1172/JCI65401. PMC 3668814. PMID 23676497.

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v t e Proteins: clusters of differentiation (see also list of human clusters of differentiation)
1–50	CD1 a-c 1A 1B 1D 1E CD2 CD3 γ δ ε CD4 CD5 CD6 CD7 CD8 a CD9 CD10 CD11 a b c d CD13 CD14 CD15 CD16 A B CD18 CD19 CD20 CD21 CD22 CD23 CD24 CD25 CD26 CD27 CD28 CD29 CD30 CD31 CD32 A B CD33 CD34 CD35 CD36 CD37 CD38 CD39 CD40 CD41 CD42 a b c d CD43 CD44 CD45 CD46 CD47 CD48 CD49 a b c d e f CD50
51–100	CD51 CD52 CD53 CD54 CD55 CD56 CD57 CD58 CD59 CD61 CD62 E L P CD63 CD64 A B C CD66 a b c d e f CD68 CD69 CD70 CD71 CD72 CD73 CD74 CD78 CD79 a b CD80 CD81 CD82 CD83 CD84 CD85 a d e h j k CD86 CD87 CD88 CD89 CD90 CD91 - CD92 CD93 CD94 CD95 CD96 CD97 CD98 CD99 CD100
101–150	CD101 CD102 CD103 CD104 CD105 CD106 CD107 a b CD108 CD109 CD110 CD111 CD112 CD113 CD114 CD115 CD116 CD117 CD118 CD119 CD120 a b CD121 a b CD122 CD123 CD124 CD125 CD126 CD127 CD129 CD130 CD131 CD132 CD133 CD134 CD135 CD136 CD137 CD138 CD140b CD141 CD142 CD143 CD144 CD146 CD147 CD148 CD150
151–200	CD151 CD152 CD153 CD154 CD155 CD156 a b c CD157 CD158 (a d e i k) CD159 a c CD160 CD161 CD162 CD163 CD164 CD166 CD167 a b CD168 CD169 CD170 CD171 CD172 a b g CD174 CD177 CD178 CD179 a b CD180 CD181 CD182 CD183 CD184 CD185 CD186 CD191 CD192 CD193 CD194 CD195 CD196 CD197 CDw198 CDw199 CD200
201–250	CD201 CD202b CD204 CD205 CD206 CD207 CD208 CD209 CDw210 a b CD212 CD213a 1 2 CD217 CD218 (a b) CD220 CD221 CD222 CD223 CD224 CD225 CD226 CD227 CD228 CD229 CD230 CD233 CD234 CD235 a b CD236 CD238 CD239 CD240CE CD240D CD241 CD243 CD244 CD246 CD247 - CD248 CD249
251–300	CD252 CD253 CD254 CD256 CD257 CD258 CD261 CD262 CD263 CD264 CD265 CD266 CD267 CD268 CD269 CD271 CD272 CD273 CD274 CD275 CD276 CD278 CD279 CD280 CD281 CD282 CD283 CD284 CD286 CD288 CD289 CD290 CD292 CDw293 CD294 CD295 CD297 CD298 CD299
301–350	CD300A CD301 CD302 CD303 CD304 CD305 CD306 CD307 CD309 CD312 CD314 CD315 CD316 CD317 CD318 CD320 CD321 CD322 CD324 CD325 CD326 CD327 CD328 CD329 CD331 CD332 CD333 CD334 CD335 CD336 CD337 CD338 CD339 CD340 CD344 CD349 CD350

v t e Proteases: metalloendopeptidases (EC 3.4.24)
ADAM proteins	Alpha secretases ADAM9 ADAM10 ADAM17 ADAM19 ADAM2 ADAM7 ADAM8 ADAM11 ADAM12 ADAM15 ADAM18 ADAM22 ADAM23 ADAM28 ADAM33 ADAMTS1 ADAMTS2 ADAMTS3 ADAMTS4 ADAMTS5 ADAMTS8 ADAMTS9 ADAMTS10 ADAMTS12 ADAMTS13
Matrix metalloproteinases	Collagenases MMP1 MMP8 Gelatinases MMP2 MMP9 MMP3 MMP7 MMP10 MMP11 MMP12 MMP13 MMP14 MMP15 MMP16 MMP17 MMP19 MMP20 MMP21 MMP23A MMP23B MMP24 MMP25 MMP26 MMP27 MMP28
Other	Neprilysin Procollagen peptidase Thermolysin Pregnancy-associated plasma protein A Bone morphogenetic protein 1 Lysostaphin Insulin-degrading enzyme ZMPSTE24

v t e Enzymes
Activity	Active site Binding site Catalytic triad Oxyanion hole Enzyme promiscuity Diffusion-limited enzyme Cofactor Enzyme catalysis
Regulation	Allosteric regulation Cooperativity Enzyme inhibitor Enzyme activator
Classification	EC number Enzyme superfamily Enzyme family List of enzymes
Kinetics	Enzyme kinetics Eadie–Hofstee diagram Hanes–Woolf plot Lineweaver–Burk plot Michaelis–Menten kinetics
Types	EC1 Oxidoreductases (list) EC2 Transferases (list) EC3 Hydrolases (list) EC4 Lyases (list) EC5 Isomerases (list) EC6 Ligases (list) EC7 Translocases (list)

ADAM10

Function

Structure

Catalytic Mechanism

Clinical significance

Brain diseases

Interaction with the malaria parasite

Breast cancer

See also

References

Further reading

External links

Navigation menu

ADAM10

Function

Structure

Catalytic Mechanism

Clinical significance

Brain diseases

Interaction with the malaria parasite

Breast cancer

See also

References

Further reading

External links

Navigation menu

Search