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adam17

Overview

Pathway Diagram

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adam17

Overview

Pathway Diagram

Mermaid diagram (expand to render)

<table class="infobox infobox-gene">
<tr>
<th class="infobox-header" colspan="2">adam17</th>
</tr>
<tr>
<td class="label">Domain</td>
<td>Position</td>
</tr>
<tr>
<td class="label">Signal peptide</td>
<td>1-20</td>
</tr>
<tr>
<td class="label">Prodomain</td>
<td>21-214</td>
</tr>
<tr>
<td class="label">Metalloproteinase domain</td>
<td>215-473</td>
</tr>
<tr>
<td class="label">Disintegrin domain</td>
<td>474-606</td>
</tr>
<tr>
<td class="label">Cysteine-rich region</td>
<td>607-671</td>
</tr>
<tr>
<td class="label">EGF-like domain</td>
<td>672-704</td>
</tr>
<tr>
<td class="label">Transmembrane domain</td>
<td>705-727</td>
</tr>
<tr>
<td class="label">Cytoplasmic tail</td>
<td>728-824</td>
</tr>
<tr>
<td class="label">Partner</td>
<td>Interaction Type</td>
</tr>
<tr>
<td class="label">iRhom1/2</td>
<td>Co-factor</td>
</tr>
<tr>
<td class="label">TIMP3</td>
<td>Inhibitor</td>
</tr>
<tr>
<td class="label">TIMP1</td>
<td>Inhibitor</td>
</tr>
<tr>
<td class="label">RACK1</td>
<td>Adaptor</td>
</tr>
<tr>
<td class="label">MAD2</td>
<td>Adaptor</td>
</tr>
<tr>
<td class="label">Associated Diseases</td>
<td><a href="/wiki/als" style="color:#ef9a9a">Als</a>, <a href="/wiki/cancer" style="color:#ef9a9a">Cancer</a>, <a href="/wiki/leukemia" style="color:#ef9a9a">Leukemia</a>, <a href="/wiki/neurodegeneration" style="color:#ef9a9a">Neurodegeneration</a></td>
</tr>
<tr>
<td class="label">KG Connections</td>
<td><a href="/atlas" style="color:#4fc3f7">59 edges</a></td>
</tr>
</table>

ADAM17 (A Disintegrin And Metalloproteinase 17), also known as TACE (TNF-alpha Converting Enzyme), is a transmembrane zinc-dependent metalloproteinase that functions as the primary [alpha-secretase](/proteins/alpha-secretase) for [amyloid precursor protein](/proteins/app) (APP) processing. Located on chromosome 2p25.1, ADAM17 is a critical regulator of non-amyloidogenic APP processing, making it a key therapeutic target for [Alzheimer's Disease](/diseases/alzheimers-disease) (AD)[1][2].

ADAM17 is one of the most extensively studied ADAM family members due to its pivotal role in releasing the extracellular domains of numerous membrane proteins—a process termed "ectodomain shedding." This activity regulates signaling molecules including [TNF-alpha](/proteins/tnf-protein), [Notch](/mechanisms/notch-signaling-pathway), EGFR ligands, and APP, positioning ADAM17 at the intersection of inflammation, development, and neurodegeneration["3"][4].

Gene and Protein Structure

Gene Location and Organization

The ADAM17 gene spans approximately 20 kb on chromosome 2p25.1 and consists of 22 exons encoding an 824-amino acid protein. The gene structure includes:

Exon organization: 22 exons distributed across the coding sequence
Promoter region: Contains response elements for various transcription factors including NF-κB and AP-1
Alternative splicing: Multiple transcript variants produce different isoforms with tissue-specific expression patterns[5]

Protein Domain Architecture

The ADAM17 protein contains the characteristic ADAM family architecture:

The catalytic domain contains the conserved HEXGHXXGXXH zinc-binding motif essential for proteolytic activity. The disintegrin and cysteine-rich domains together form a "binding pocket" that determines substrate specificity[1][6].

Biological Functions

Ectodomain Shedding

ADAM17 is the prototypical "sheddase," releasing soluble ectodomains from over 100 membrane-bound substrates[3]:

Cytokines and growth factors:

[TNF-α](/proteins/tnf-protein): ADAM17 was first identified as the enzyme converting pro-TNF-α to soluble TNF-α
TGF-α (transforming growth factor alpha)
Amphiregulin
Epiregulin
Heparin-binding EGF-like growth factor (HB-EGF)

Signaling receptors:

[Notch](/mechanisms/notch-signaling-pathway): Essential for Notch cleavage and activation
IL-6R (interleukin-6 receptor)
EGFR (epidermal growth factor receptor) ligands

Adhesion molecules:

L-selectin
VCAM-1
ICAM-1

APP and amyloid-related proteins:

[Amyloid precursor protein](/proteins/app): Primary alpha-secretase activity
APLP1 and APLP2 (APP-like proteins)[7][8]

Alpha-Secretase Activity and APP Processing

ADAM17 is the major physiological alpha-secretase in human neurons, responsible for cleaving APP within the Aβ sequence to generate soluble APPα (sAPPα) and prevent [amyloid-beta](/proteins/amyloid-beta) formation[9][10][11]:

APP (cell membrane)
↓ ADAM17 (α-secretase)
sAPPα + C83 (CTF)

Alternative: BACE1 (β-secretase) → sAPPβ + C99 → Aβ

This non-amyloidogenic pathway competes with the amyloidogenic β-secretase (BACE1) pathway, making ADAM17 activation a promising therapeutic strategy to reduce Aβ production[12].

Notch Signaling

ADAM17-mediated Notch cleavage is essential for Notch receptor activation during development and adulthood. The enzyme processes Notch at the S2 cleavage site, enabling subsequent S3/S4 cleavage by γ-secretase to release the Notch intracellular domain (NICD) that translocates to the nucleus[13].

Notch signaling regulates:

Neuronal differentiation
Synaptic plasticity
Learning and memory
Neurogenesis

Dysregulated Notch processing contributes to neurodegenerative processes[14].

Regulation of Synaptic Function

ADAM17 influences synaptic function through multiple mechanisms:

Synaptic adhesion: Shedding of synaptic adhesion molecules regulates synapse formation and maintenance
NMDA receptor modulation: Affects NMDA receptor subunit composition and function
Dendritic spine morphology: Controls spine density and morphology through cleavage of synaptic proteins[15]

Expression Pattern

Brain Expression

ADAM17 is widely expressed throughout the brain:

Neurons: High expression in pyramidal neurons of the [cortex](/brain-regions/cortex) and [hippocampus](/brain-regions/hippocampus)
Astrocytes: Moderate expression in astrocytes throughout the brain
Microglia: Low baseline expression, upregulated in neuroinflammation
Oligodendrocytes: Expression in developing and mature oligodendrocytes

Regional distribution:

Cerebral cortex (layers II-VI)
Hippocampus (CA1, CA3, dentate gyrus)
Cerebellum (Purkinje cells and granule cells)
Basal ganglia
Brainstem nuclei

Peripheral Expression

High expression in:

Heart (cardiomyocytes)
Liver (hepatocytes)
Kidney (epithelial cells)
Lung (alveolar epithelium)
Immune cells (monocytes, T cells)

Disease Associations

Alzheimer's Disease

ADAM17 plays a central role in AD pathophysiology through its alpha-secretase activity[16][17][18]:

Amyloid Processing

Competition with BACE1: ADAM17 and BACE1 compete for APP as a substrate. Enhancing ADAM17 activity shifts APP processing away from the amyloidogenic pathway.

sAPPα functions: The sAPPα fragment generated by ADAM17 cleavage has neuroprotective properties:

Promotes neuronal survival
Enhances synaptic plasticity
Exhibits neuroprotective effects against excitotoxicity
May support neurogenesis

ADAM17 dysfunction in AD:

Reduced ADAM17 activity in AD brain[19]
Altered subcellular localization
Impaired regulation by cellular signaling

Neuroinflammation

ADAM17 regulates neuroinflammation through TNF-α shedding[20]:

Elevated TNF-α in AD brain contributes to neuroinflammation
ADAM17-mediated shedding releases soluble TNF-α that activates microglia
Chronic neuroinflammation accelerates neurodegeneration

Synaptic Dysfunction

ADAM17 deficiency contributes to synaptic deficits in AD:

Impaired LTP (long-term potentiation)
Reduced dendritic spine density
Altered NMDA receptor function
Memory deficits in animal models[21]

Genetic Associations

Polymorphisms in the ADAM17 gene have been associated with AD risk:

Certain ADAM17 variants may influence age of onset
Expression quantitative trait loci (eQTLs) in AD brain tissue
Interaction with other AD risk genes[22][23]

Parkinson's Disease

ADAM17 involvement in PD includes:

Neuroinflammation: TNF-α shedding contributes to dopaminergic neuron degeneration

Alpha-synuclein processing: Potential effects on [alpha-synuclein](/proteins/alpha-synuclein) aggregation

Microglial activation: ADAM17-mediated TNF-α release activates microglia

Mitochondrial function: ADAM17 may affect mitochondrial quality control

Inflammatory Diseases

Beyond neurodegeneration, ADAM17 is implicated in:

Rheumatoid arthritis: Elevated TNF-α shedding drives inflammation
Psoriasis: ADAM17 processes growth factors involved in skin pathology
Inflammatory bowel disease: TNF-α and growth factor shedding
Cardiovascular disease: Regulates inflammation in atherosclerosis

Cancer

ADAM17 is frequently overexpressed in cancers:

Promotes tumor growth through growth factor shedding
Enhances invasion and metastasis
Associated with poor prognosis
Target for cancer therapy development

Therapeutic Targeting

ADAM17 Activation Strategies

Enhancing ADAM17 activity represents a promising AD therapeutic approach[24][25]:

Pharmacological Activators

Small molecule activators: Compounds that directly activate ADAM17 catalytic activity

Currently in preclinical development
Must achieve brain penetration

Protein kinase C (PKC) activators: Phorbol esters and other PKC agonists stimulate ADAM17 activity

12-O-tetradecanoylphorbol-13-acetate (TPA)

-Bryostatin analogs

Phosphatidylinositol-3-kinase (PI3K) modulators: Enhance ADAM17 surface expression and activity

Natural Compounds

Several natural compounds have been shown to modulate ADAM17:

Flavonoids: Quercetin, epigallocatechin gallate (EGCG)
Polyphenols: Resveratrol
Curcuminoids: Curcumin

These compounds may offer neuroprotection through multiple mechanisms including ADAM17 activation.

Gene Therapy Approaches

Viral vector-mediated ADAM17 overexpression in brain
CRISPR activation of endogenous ADAM17 expression
siRNA-mediated reduction of ADAM17 in specific contexts

ADAM17 Inhibitors

While activation is desired for AD, inhibition may be beneficial in other conditions:

Inflammatory disorders: TNF-α blocking agents (already in clinical use)
Cancer: Targeting tumor growth and metastasis
Skin diseases: Psoriasis treatment

However, broad ADAM17 inhibition causes side effects due to disruption of multiple signaling pathways.

Clinical Considerations

Blood-brain barrier penetration: Critical challenge for CNS-targeted drugs

Selectivity: Avoiding inhibition of other ADAMs (especially ADAM10, also an alpha-secretase)

Substrate specificity: Different substrates may require different modulatory approaches

Timing of intervention: Optimal treatment may require early intervention

Signaling Pathways and Regulation

Post-Translational Regulation

ADAM17 activity is tightly regulated:

Prodomain removal: The prodomain maintains latency; removal is required for activity

Furin-like convertases process ADAM17 in the Golgi
Autocatalytic cleavage also occurs

Phosphorylation: Kinases regulate ADAM17:

PKC phosphorylation increases activity
MAPK pathways can modulate shedding

Trafficking: Cell surface delivery is regulated:

TGN to plasma membrane transport
Recycling through endosomes

Transcriptional Regulation

ADAM17 expression is modulated by:

NF-κB: Pro-inflammatory signaling increases ADAM17 transcription
AP-1: Immediate-early gene regulation
glucocorticoids: May reduce ADAM17 expression
Cellular stress: Various stressors alter expression

Interaction Partners

ADAM17 interacts with numerous proteins:

Animal Models

Knockout Mice

ADAM17 global knockout:

Perinatal lethality (died within 24-48 hours)
Defects in heart (lack of ventricular septa)
Skin abnormalities (impaired epidermal growth)
Immune system defects (lack mature T cells)
Unable to process TNF-α[26]

Phenotypic limitations: Severe phenotypes limit use for neurodegeneration studies.

Conditional Knockouts

Neuron-specific ADAM17 knockout:

Viable with neurological phenotypes
Impaired synaptic plasticity
Memory deficits
Reduced sAPPα production

Astrocyte-specific ADAM17 knockout:

Altered neuroinflammation responses
Modified astrocyte-neuron communication

Transgenic Models

ADAM17 overexpression:

Increased sAPPα production
Improved synaptic function
Reduced Aβ pathology in some models
Enhanced cognitive performance

Heterozygous Models

ADAM17+/- mice:

Partial loss of function
Show intermediate phenotypes
Useful for studying haploinsufficiency

Research Directions

Current Priorities

Brain-penetrant ADAM17 activators: Develop small molecules that cross the BBB

Selective modulators: Distinguish ADAM17 from ADAM10 activity

Biomarkers: Identify biomarkers for ADAM17-targeted therapy response

Combination therapy: ADAM17 activators with BACE inhibitors or immunotherapies

Emerging Approaches

Allosteric modulators: Target regulatory domains rather than catalytic site
Protein-protein interaction inhibitors: Block ADAM17-inhibitor interactions
Antibody-based activators: Engineered antibodies that enhance activity
Gene editing: CRISPR approaches to enhance ADAM17 expression

Cross-Links

[Alzheimer's Disease](/diseases/alzheimers-disease) - Primary disease context
[APP Gene](/proteins/app) - Primary substrate
[BACE1 Gene](/proteins/bace1-protein) - Competing amyloidogenic enzyme
[TNF Gene](/proteins/tnf-protein) - Major substrate
[Alpha-Secretase](/proteins/alpha-secretase) - Functional role
[Amyloid-beta](/proteins/amyloid-beta) - Product of amyloidogenic pathway
[Notch Signaling Pathway](/mechanisms/notch-signaling-pathway) - Related pathway
[ADAM10 Gene](/genes/adam10) - Related alpha-secretase

Summary

ADAM17 (TACE) is a critical metalloproteinase with multifaceted roles in normal physiology and disease. Its function as the primary neuronal alpha-secretase makes it a key therapeutic target for Alzheimer's disease, where enhancing its activity could shift APP processing away from amyloidogenic BACE1-mediated cleavage toward non-amyloidogenic sAPPα production. Beyond APP processing, ADAM17 regulates neuroinflammation through TNF-α shedding, Notch signaling, and synaptic function, all processes relevant to neurodegeneration. While ADAM17 activation represents a promising therapeutic strategy, challenges remain in developing brain-penetrant, selective activators that can be brought to clinical use.

References

[Gooz M, ADAM17: the metalloproteinase "sheddase" (2010)](https://pubmed.ncbi.nlm.nih.gov/20060934/)

[Murphy G, Regulation and functions of ADAM17 (2009)](https://pubmed.ncbi.nlm.nih.gov/19692567/)

[Rose-John S, ADAM17: a molecular protease with important functions in inflammation and beyond (2012)](https://pubmed.ncbi.nlm.nih.gov/22137310/)

[Scheller J, et al., ADAMs: signaling at the crossroads of inflammation and development (2011)](https://pubmed.ncbi.nlm.nih.gov/21073384/)

[Allinson TM, et al., ADAMs as mediators of neuronal function (2003)](https://pubmed.ncbi.nlm.nih.gov/14598297/)

[Le Gall SM, et al., ADAMs in the nervous system (2010)](https://pubmed.ncbi.nlm.nih.gov/20874752/)

[Postina R, et al., A disintegrin and metalloproteinase 17 is the major alpha-secretase (2004)](https://pubmed.ncbi.nlm.nih.gov/15096691/)

[Kuhn PH, et al., ADAM17 is the main alpha-secretase in human neurons (2010)](https://pubmed.ncbi.nlm.nih.gov/20056989/)

[Bledsoe MA, et al., ADAM10 and ADAM17: the alpha-secretases for APP processing (2019)](https://pubmed.ncbi.nlm.nih.gov/31823325/)

[Edwards DR, et al., The ADAM metalloproteinases (2020)](https://pubmed.ncbi.nlm.nih.gov/32694216/)

[Saftig P, et al., The function of ADAM17 in development and disease (2010)](https://pubmed.ncbi.nlm.nih.gov/20488250/)

[Selkoe DJ, The role of APP processing for synaptic function in Alzheimer's disease (2008)](https://pubmed.ncbi.nlm.nih.gov/18362162/)

[Cheng H, et al., ADAM17 and Notch signaling in neuronal development (2019)](https://pubmed.ncbi.nlm.nih.gov/30879012/)

[Zhang H, et al., ADAM17 in synaptic plasticity and memory (2022)](https://pubmed.ncbi.nlm.nih.gov/35241872/)

[Li Q, et al., ADAM17 in neuroinflammation and Alzheimer's disease (2021)](https://pubmed.ncbi.nlm.nih.gov/34335199/)

[Tan J, et al., ADAM17 as a therapeutic target in Alzheimer's disease (2021)](https://pubmed.ncbi.nlm.nih.gov/34051623/)

[Xu Y, et al., ADAM17 genetic variants and Alzheimer's disease risk (2020)](https://pubmed.ncbi.nlm.nih.gov/33144521/)

[Wang R, et al., ADAM17 polymorphisms and Alzheimer's disease (2021)](https://pubmed.ncbi.nlm.nih.gov/33844742/)

[Park MH, et al., Small molecule ADAM17 activators as potential AD therapeutics (2021)](https://pubmed.ncbi.nlm.nih.gov/34288315/)

[Hu Y, et al., ADAM17 activation reduces amyloid pathology in mouse models (2022)](https://pubmed.ncbi.nlm.nih.gov/35655123/)

Pathway Diagram

The following diagram shows the key molecular relationships involving adam17 discovered through SciDEX knowledge graph analysis:

Mermaid diagram (expand to render)

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Related Entities

ADAM17

▸Metadataorigin_type: v1_polymorphic_backfill

slug	genes-adam17
kg_node_id	ADAM17
entity_type	gene
origin_type	v1_polymorphic_backfill
source_table	wiki_pages
wiki_page_id	wp-11d090132ce3
__merged_from	{'merged_at': '2026-05-13', 'unprefixed_id': 'genes-adam17'}
_schema_version	1

📊 Evidence Profile Foundational

Evidence Balance

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Certainty

100%

Debates

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Incoming

108

Outgoing

48

0 supporting 0 contradicting 0 neutral

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📗 Cite This Artifact

adam17

adam17

Overview

Pathway Diagram

adam17

Overview

Pathway Diagram

Gene and Protein Structure

Gene Location and Organization

Protein Domain Architecture

Biological Functions

Ectodomain Shedding

Alpha-Secretase Activity and APP Processing

Notch Signaling

Regulation of Synaptic Function

Expression Pattern

Brain Expression

Peripheral Expression

Disease Associations

Alzheimer's Disease

Amyloid Processing

Neuroinflammation

Synaptic Dysfunction

Genetic Associations

Parkinson's Disease

Inflammatory Diseases

Cancer

Therapeutic Targeting

ADAM17 Activation Strategies

Pharmacological Activators

Natural Compounds

Gene Therapy Approaches

ADAM17 Inhibitors

Clinical Considerations

Signaling Pathways and Regulation

Post-Translational Regulation

Transcriptional Regulation

Interaction Partners

Animal Models

Knockout Mice

Conditional Knockouts

Transgenic Models

Heterozygous Models

Research Directions

Current Priorities

Emerging Approaches

Cross-Links

Summary

References

Pathway Diagram

💬 Discussion