TRPM4 Gene

TRPM4 Gene

<div class="infobox infobox-gene">
<table>
<tr><th colspan="2">TRPM4</th></tr>
<tr><td>Symbol</td><td>TRPM4</td></tr>
<tr><td>Full Name</td><td>Transient Receptor Potential Cation Channel Subfamily M Member 4</td></tr>
<tr><td>Chromosome</td><td>19q13.33</td></tr>
<tr><td>NCBI Gene ID</td><td>[54795](https://www.ncbi.nlm.nih.gov/gene/54795)</td></tr>
<tr><td>OMIM</td><td>[606071](https://omim.org/entry/606071)</td></tr>
<tr><td>Ensembl</td><td>[ENSG00000130589](https://www.ensembl.org/Homo_sapiens/Gene/Summary?g=ENSG00000130589)</td></tr>
<tr><td>UniProt</td><td>[Q9HCF6](https://www.uniprot.org/uniprot/Q9HCF6)</td></tr>
<tr><td>Aliases</td><td>TRPM4, LTrp4, FLJ90167</td></tr>
<tr>
<td class="label">KG Connections</td>
<td><a href="/atlas" style="color:#4fc3f7">1 edges</a></td>
</tr>
</table>
</div>

Overview

TRPM4 encodes transient receptor potential cation channel subfamily M member 4, a calcium-activated non-selective cation channel that plays critical roles in various physiological processes. Unlike other TRP channels, TRPM4 is impermeable to calcium — it conducts monovalent cations (primarily Na⁺) and is directly activated by intracellular calcium[@nilius2007][@birnbaumer2009].

TRPM4 Gene

<div class="infobox infobox-gene">
<table>
<tr><th colspan="2">TRPM4</th></tr>
<tr><td>Symbol</td><td>TRPM4</td></tr>
<tr><td>Full Name</td><td>Transient Receptor Potential Cation Channel Subfamily M Member 4</td></tr>
<tr><td>Chromosome</td><td>19q13.33</td></tr>
<tr><td>NCBI Gene ID</td><td>[54795](https://www.ncbi.nlm.nih.gov/gene/54795)</td></tr>
<tr><td>OMIM</td><td>[606071](https://omim.org/entry/606071)</td></tr>
<tr><td>Ensembl</td><td>[ENSG00000130589](https://www.ensembl.org/Homo_sapiens/Gene/Summary?g=ENSG00000130589)</td></tr>
<tr><td>UniProt</td><td>[Q9HCF6](https://www.uniprot.org/uniprot/Q9HCF6)</td></tr>
<tr><td>Aliases</td><td>TRPM4, LTrp4, FLJ90167</td></tr>
<tr>
<td class="label">KG Connections</td>
<td><a href="/atlas" style="color:#4fc3f7">1 edges</a></td>
</tr>
</table>
</div>

Overview

TRPM4 encodes transient receptor potential cation channel subfamily M member 4, a calcium-activated non-selective cation channel that plays critical roles in various physiological processes. Unlike other TRP channels, TRPM4 is impermeable to calcium — it conducts monovalent cations (primarily Na⁺) and is directly activated by intracellular calcium[@nilius2007][@birnbaumer2009].

TRPM4 is expressed in numerous tissues including the heart, immune system, and brain. In the heart, it is crucial for cardiac electrical conduction. In the immune system, it regulates T cell activation and other immune responses. In the brain, it is implicated in various neurological conditions including multiple sclerosis, stroke, and potentially neurodegenerative diseases[@guinamard2014][@vlasov2018].

Normal Function

Channel Properties

TRPM4 is a voltage-dependent, calcium-activated monovalent cation channel with several distinctive properties:

Regulation

TRPM4 activity is modulated by multiple mechanisms:

• Intracellular calcium — Primary activator
• Voltage — Depolarization increases open probability
• Phosphorylation — PKC and CaM kinase II can modulate activity
• ATP — Intracellular ATP can inhibit the channel
• pH — Intracellular pH affects channel function
• Calmodulin — Mediates Ca²⁺-dependent activation

Physiological Roles

Cardiovascular System

In the heart, TRPM4 plays essential roles in cardiac electrophysiology[@barbold2009][@bauer2012]:

Immune System

TRPM4 is expressed in various immune cells and regulates:

• T cell activation — Calcium-dependent activation signals
• B cell function — BCR signaling modulation
• Dendritic cell migration — Chemotaxis
• Macrophage function — Inflammatory responses

Nervous System

In neurons and glia, TRPM4 contributes to[@wang2021][@jang2020]:

• Neuronal excitability — Modulates resting membrane potential
• Synaptic transmission — Affects neurotransmitter release
• Neuroprotection — Some evidence for protective roles
• Neuroinflammation — Regulates microglial activation

Expression Pattern

TRPM4 exhibits broad tissue expression:

High Expression

• Heart — Atria, ventricles, conduction system
• T cells — Activated T lymphocytes
• Brain — Cortex, hippocampus, cerebellum
• Kidney — Various tubular segments

Moderate Expression

• Spleen — Immune cells
• Lung — Epithelial cells
• Placenta — Various cell types
• Pancreas — Islet cells

Low Expression

• Liver — Low levels
• Skeletal muscle — Minimal

Cellular Localization

• Plasma membrane — Primary location
• Endoplasmic reticulum — Some evidence
• Neuronal processes — Axons and dendrites

Disease Associations

Cardiac Conduction Disorders

TRPM4 gain-of-function mutations cause progressive familial heart block[@barbold2009][@bauer2011]:

Progressive Familial Heart Block Type 1 (PFHB1):

• Autosomal dominant inheritance
• Progressive AV conduction disease — From first-degree to complete block
• Atrial fibrillation — Increased risk
• Syncope — Due to bradyarrhythmias
• Pacemaker requirement — Often needed by fourth decade

• Mutant channels show increased activity
• Enhanced depolarization in conduction system
• Progressive conduction system dysfunction

Multiple Sclerosis and EAE

TRPM4 plays a complex role in neuroinflammation[@schattling2012][@schattling2016]:

Experimental Autoimmune Encephalomyelitis (EAE):

• Increased TRPM4 expression in microglia and neurons during EAE
• Axonal degeneration — TRPM4 contributes to axonal loss
• Neuronal death — Channel mediates excitotoxic damage
• Therapeutic potential — TRPM4 inhibition may be protective

• TRPM4 expression increased in active lesions
• Associated with demyelination and axonal damage
• Potential biomarker and therapeutic target

Stroke and Ischemia

TRPM4 is implicated in stroke pathophysiology[@simon2018]:

Ischemic injury:

• TRPM4 activity increases during ischemia
• Contributes to ionic dysregulation
• Aggravates neuronal death
• Blocking TRPM4 is neuroprotective in models

• Involved in blood-brain barrier disruption
• Modulates edema formation

Parkinson's Disease

Emerging evidence links TRPM4 to PD[@krishnan2020]:

• Dopaminergic neurons — TRPM4 expressed in substantia nigra
• α-Synuclein interaction — May affect neuronal vulnerability
• Oxidative stress — TRPM4 may be involved in stress responses
• Therapeutic potential — Targeting TRPM4 may protect neurons

Microglial TRPM4

TRPM4 in microglia plays a critical role in neuroinflammation[@chen2023]:

• Pro-inflammatory activation — TRPM4 contributes to microglial activation
• Cytokine release — TRPM4 regulates release of inflammatory mediators
• Neurotoxicity — Microglial TRPM4 can mediate neurotoxic effects
• Therapeutic targeting — TRPM4 inhibition may reduce neuroinflammation

Genetic Variants

TRPM4 genetic variants are associated with disease phenotypes[@simpson2023]:

• Cardiac conduction variants — Specific SNPs linked to AV block
• Population genetics — Variant frequencies across populations
• Functional studies — How variants affect channel function
• Clinical significance — Implications for risk stratification

Other Neurological Conditions

• Epilepsy — Altered expression in seizure models
• Migraine — Possible role in trigeminovascular system
• Neuropathic pain — Involvement in pain signaling

Neuronal Excitability

TRPM4 significantly impacts neuronal excitability through sodium handling[@yamamoto2024]:

• Resting membrane potential — TRPM4 contributes to setting resting potential
• Action potential dynamics — TRPM4 modulates action potential shape
• Firing patterns — TRPM4 influences neuronal firing frequency
• Excitotoxicity — TRPM4 can exacerbate excitotoxic damage

Therapeutic Development

Novel TRPM4-targeted therapies are under development[@liu2024]:

• Small molecule inhibitors — Clinical candidates in development
• Peptide blockers — Novel peptide-based inhibitors
• Allosteric modulators — Positive and negative allosteric modulators
• Gene therapy — Silencing approaches for specific applications

Therapeutic Implications

Drug Development

TRPM4 is a potential drug target for multiple conditions[@vlasov2018]:

Cardiovascular Applications

• Antiarrhythmic drugs — TRPM4 blockers for certain arrhythmias
• Heart failure — Modulating conduction system function

Neurological Applications

• Neuroprotection — TRPM4 inhibitors in stroke and trauma
• MS therapy — Targeting neuroinflammation
• PD prevention — Protecting dopaminergic neurons

Immunomodulation

• Autoimmune diseases — Modulating T cell responses
• Transplant rejection — Immune suppression strategies

Current Research Status

• Small molecule inhibitors — Being developed and tested
• Gene therapy approaches — Targeting TRPM4 expression
• Combination strategies — TRPM4 modulators with other therapies

Mechanisms of Disease

Cardiac Conduction

TRPM4 mutations cause conduction disease through:

Neuroinflammation

TRPM4 contributes to neuroinflammation through:

Ischemic Injury

During stroke, TRPM4 contributes to:

Animal Models

• Trpm4 knockout mice — Viable with cardiac and immune phenotypes
• Transgenic overexpression — Cardiac-specific effects
• Disease models — EAE, stroke, cardiac conduction disease

Key Publications

TRPM4 Channel Structure and Biophysics

Protein Architecture

TRPM4 is a member of the melastatin subfamily of TRP channels, characterized by its unique structure[@birnbaumer2009]:

Transmembrane Domain:

• Six transmembrane helices (S1-S6)
• Pore loop between S5 and S6 helices
• Voltage sensor domain (S1-S4)

• Multiple ankyrin repeat domains (ARD)
• Required for channel tetramerization
• Mediates protein-protein interactions

• Coil-coil domains for tetramer formation
• Calmodulin binding site
• ATP binding site

Ion Selectivity and Conductance

TRPM4 has distinctive biophysical properties[@nilius2007]:

Selectivity Filter:

• Non-selective for monovalent cations
• Permeates Na⁺, K⁺, Cs⁺ equally well
• Impermeable to divalent cations (Ca²⁺, Mg²⁺)
• Single channel conductance: ~75 pS

• Strongly voltage-dependent activation
• Gates open with depolarization
• V½ ≈ +40 mV in physiological conditions

• Direct activation by intracellular Ca²⁺
• Activation threshold: 1-10 μM
• Calmodulin mediates Ca²⁺ sensitivity

Gating Mechanisms

TRPM4 gating involves multiple regulatory mechanisms:

Calcium-Dependent Gating:

• Ca²⁺ binds to N-terminal domain
• Calmodulin modulates sensitivity
• Desensitization with prolonged Ca²⁺ exposure

• Voltage sensor couples to gate
• Depolarization increases open probability
• S4 helix contains voltage sensors

• ATP: inhibitory at millimolar concentrations
• pH: acidic pH reduces activity
• Phosphorylation: PKC enhances activity

TRPM4 in Cellular Physiology

Cardiac Electrophysiology

TRPM4 plays crucial roles in cardiac electrical function[@barbold2009][@bauer2012]:

Sinoatrial Node Function:

• Contributes to pacemaker depolarization
• Regulates heart rate through Na⁺ influx
• Modulates automaticity

• Influences AV node conduction velocity
• Affects PR interval on ECG
• May contribute to AV block

• Modulates His-Purkinje conduction
• Affects ventricular activation
• Contributes to cardiac remodeling

• Gain-of-function mutations cause heart block
• Enhanced TRPM4 activity leads to conduction disease
• Potential antiarrhythmic target

Immune System Regulation

TRPM4 is essential for immune cell function[@krishnan2020]:

T Cell Activation:

• Calcium influx during T cell receptor engagement
• Required for full activation
• Modulates cytokine production

• Regulates chemotaxis
• Affects antigen presentation
• Guides immune surveillance

• Modulates inflammatory responses
• Regulates phagocytosis
• Controls cytokine release

• Affects B cell receptor signaling
• Influences antibody production
• May affect autoimmunity

Neuronal Physiology

In the nervous system, TRPM4 regulates[@wang2021][@jang2020]:

Membrane Potential:

• Contributes to resting membrane potential
• Modulates neuronal excitability
• Affects action potential threshold

• Regulates neurotransmitter release
• Modulates synaptic vesicle dynamics
• Influences synaptic plasticity

• Present in astrocytes and microglia
• Affects glutamate clearance
• Modulates neuroinflammation

TRPM4 in Neurodegenerative Diseases

Parkinson's Disease

TRPM4 has emerging relevance to PD[@krishnan2020]:

Dopaminergic Neurons:

• TRPM4 is expressed in substantia nigra
• Regulates neuronal calcium homeostasis
• May influence vulnerability to stress

• Possible interaction with α-synuclein aggregates
• May affect neuronal susceptibility
• Therapeutic targeting being explored

• TRPM4 responds to oxidative stress
• May contribute to cell death pathways
• Modulation may provide neuroprotection

Multiple Sclerosis

TRPM4 plays a complex role in MS[@schattling2012][@schattling2016]:

EAE Model Studies:

• TRPM4 expression increases during EAE
• Contributes to axonal degeneration
• Mediates neuronal loss

• TRPM4 in activated microglia
• Regulates cytokine release
• Affects demyelination

• TRPM4 inhibition may be protective
• Potential disease-modifying target
• Biomarker potential for disease activity

Stroke and Ischemia

TRPM4 is implicated in stroke pathophysiology[@simon2018]:

Ischemic Injury:

• Activity increases during ischemia
• Contributes to ionic dysregulation
• Aggravates neuronal death

• Blocking TRPM4 is neuroprotective in models
• Reduces infarct size
• Improves functional recovery

• Involved in blood-brain barrier disruption
• Modulates edema formation
• Affects inflammatory responses

Epilepsy

TRPM4 may be involved in seizure disorders:

Seizure Models:

• Altered expression in experimental epilepsy
• Contributes to hyperexcitability
• Possible therapeutic target

• Affects neuronal membrane properties
• Modulates calcium homeostasis
• Influences neurotransmitter release

Therapeutic Targeting

Drug Development

TRPM4 is a promising drug target[@gerhold2021]:

Inhibitor Development:

• Small molecule TRPM4 blockers in development
• Virtual screening approaches
• Structure-activity relationship studies

• Developing selective inhibitors is challenging
• TRPM4 shares structural features with other TRP channels
• Need for subtype-selective compounds

• Several compounds in preclinical development
• Optimization for brain penetration
• Safety profiling underway

Therapeutic Applications

Cardiovascular:

• TRPM4 blockers for arrhythmias
• Treatment for progressive heart block
• Prevention of atrial fibrillation

• Neuroprotection in stroke
• MS disease modification
• PD prevention strategies

• Modulating T cell responses
• Autoimmune disease treatment
• Transplant rejection prevention

Genetics and Variants

Disease-Causing Mutations

TRPM4 mutations cause human disease[@choi2020]:

Progressive Familial Heart Block Type 1 (PFHB1):

• Autosomal dominant inheritance
• Gain-of-function mutations
• Progressive conduction system disease

• A433T (most common)
• R498W
• V351I
• L888P

• Mutant channels have increased open probability
• Enhanced depolarization in conduction system
• Progressive degeneration

Genetic Variants and Susceptibility

Polymorphisms may affect disease risk:

Population Studies:

• Certain SNPs associated with arrhythmia risk
• May affect drug response
• Implications for personalized medicine

• Some variants affect channel trafficking
• Others alter gating properties
• May influence disease severity

TRPM4 in Animal Models

Knockout Mouse Studies

Genetic mouse models reveal TRPM4 function:

Trpm4⁻/⁻ Mice:

• Viable and fertile
• Cardiac phenotypes: bradycardia
• Immune phenotypes: impaired T cell activation

• Reduced cardiac conduction velocity
• Impaired immune responses
• Altered neuronal excitability

Transgenic Models

Overexpression models:

Cardiac-Specific Overexpression:

• Conduction system dysfunction
• Atrial fibrillation
• Heart failure

• Increased seizure susceptibility
• Altered synaptic transmission
• Neuroinflammatory changes

Disease Models

TRPM4 in disease-specific models:

EAE Model:

• TRPM4 contributes to demyelination
• Blocking improves outcomes
• Therapeutic mechanism

• TRPM4 knockout reduces injury
• TRPM4 inhibition is protective
• Mechanism: reduced ionic dysregulation

Research Directions

Key questions remain:

See Also

Key questions remain:

See Also

• [Ion Channels in the Heart](/mechanisms/ion-channels-cardiac)
• [Multiple Sclerosis](/diseases/multiple-sclerosis)
• [Parkinson's Disease](/diseases/parkinsons-disease)
• [Stroke](/diseases/stroke)
• [TRP Channels](/mechanisms/trp-channels)

External Links

• [NCBI Gene: TRPM4](https://www.ncbi.nlm.nih.gov/gene/54795)
• [OMIM: 606071](https://omim.org/entry/606071)
• [UniProt: Q9HCF6](https://www.uniprot.org/uniprot/Q9HCF6)
• [Ensembl: ENSG00000130589](https://www.ensembl.org/Homo_sapiens/Gene/Summary?g=ENSG00000130589)
• [IUPHAR: TRPM4](https://www.guidetopharmacology.org/GRAC/ObjectDisplayForward?objectId=507)

References