ramp1-protein

RAMP1 (Receptor Activity Modifying Protein 1) Protein

<div class="infobox infobox-protein">
| | |
|---|---|
| Protein Name | Receptor Activity Modifying Protein 1 (RAMP1) |
| Gene | [RAMP1](/genes/ramp1) |
| UniProt ID | [O60883](https://www.uniprot.org/uniprot/O60883) |
| Molecular Weight | ~17.5 kDa (175 amino acids) |
| Subcellular Localization | Plasma membrane, Endoplasmic reticulum |
| Protein Family | RAMP family (RAMP1, RAMP2, RAMP3) |
| Chromosomal Location | 2q36.1 |
| Brain Expression | High in trigeminal ganglion, cortex, hippocampus |
</div>

Overview

Receptor Activity Modifying Protein 1 (RAMP1) is a single-pass membrane protein that is essential for forming functional calcitonin gene-related peptide (CGRP) receptors. RAMP1 belongs to a small family of receptor activity-modifying proteins that dictate ligand specificity and trafficking of the calcitonin receptor family[@poe2019][@russell2020].

The RAMP family consists of three members (RAMP1, RAMP2, and RAMP3) that each confer distinct pharmacology when co-expressed with either the calcitonin receptor (CALCR) or the calcitonin receptor-like receptor (CALCRL). RAMP1 specifically partners with CALCRL to create the canonical CGRP receptor (CALCRL/RAMP1), while CALCRL/RAMP2 forms the adrenomedullin receptor, and CALCRL/RAMP3 creates an alternate adrenomedullin receptor[@hay2020].

In the nervous system, CGRP signaling through RAMP1-containing receptors plays critical roles in:

RAMP1 (Receptor Activity Modifying Protein 1) Protein

<div class="infobox infobox-protein">
| | |
|---|---|
| Protein Name | Receptor Activity Modifying Protein 1 (RAMP1) |
| Gene | [RAMP1](/genes/ramp1) |
| UniProt ID | [O60883](https://www.uniprot.org/uniprot/O60883) |
| Molecular Weight | ~17.5 kDa (175 amino acids) |
| Subcellular Localization | Plasma membrane, Endoplasmic reticulum |
| Protein Family | RAMP family (RAMP1, RAMP2, RAMP3) |
| Chromosomal Location | 2q36.1 |
| Brain Expression | High in trigeminal ganglion, cortex, hippocampus |
</div>

Overview

Receptor Activity Modifying Protein 1 (RAMP1) is a single-pass membrane protein that is essential for forming functional calcitonin gene-related peptide (CGRP) receptors. RAMP1 belongs to a small family of receptor activity-modifying proteins that dictate ligand specificity and trafficking of the calcitonin receptor family[@poe2019][@russell2020].

The RAMP family consists of three members (RAMP1, RAMP2, and RAMP3) that each confer distinct pharmacology when co-expressed with either the calcitonin receptor (CALCR) or the calcitonin receptor-like receptor (CALCRL). RAMP1 specifically partners with CALCRL to create the canonical CGRP receptor (CALCRL/RAMP1), while CALCRL/RAMP2 forms the adrenomedullin receptor, and CALCRL/RAMP3 creates an alternate adrenomedullin receptor[@hay2020].

In the nervous system, CGRP signaling through RAMP1-containing receptors plays critical roles in:

• Migraine pathogenesis (the primary target of CGRP monoclonal antibodies and gepants)
• Neuroprotection against ischemic injury
• Modulation of pain transmission
• Regulation of neuroinflammation
• Potential involvement in Alzheimer's disease and other neurodegenerative conditions

Gene and Protein Structure

Gene Organization

The human RAMP1 gene is located on chromosome 2q36.1 and encodes a 175-amino acid protein. The gene consists of 4 exons spanning approximately 6 kb. The gene is expressed in various tissues, with highest levels in the trigeminal ganglion, dorsal root ganglia, and specific brain regions.

Protein Domain Architecture

RAMP1 is a small type I membrane protein with a distinctive structure:

N-terminal Extracellular Domain (aa 1-100): This relatively long extracellular domain contains:

• A signal peptide (aa 1-20)
• Two N-linked glycosylation sites (Asn-47, Asn-64)
• A conserved cysteine pair that forms a disulfide bond
• The C-terminal portion of this domain directly contacts CGRP and determines ligand specificity

Intracellular C-terminal Tail (aa 120-175): Short cytoplasmic tail containing:

• A dileucine sorting motif
• Potential phosphorylation sites
• Interaction sites for intracellular proteins

Post-translational Modifications

RAMP1 undergoes several post-translational modifications:

• N-linked glycosylation: Essential for proper folding, trafficking, and function
• Disulfide bond formation: Required for structural integrity
• Palmitoylation: Possible at cysteine residues near the transmembrane domain
• Dimerization: RAMP1 can form homodimers, though the functional significance is unclear

Normal Physiological Functions

CGRP Receptor Formation

RAMP1's primary function is to enable CGRP receptor formation:

Receptor Assembly: RAMP1 forms a heterodimeric complex with CALCRL. This complex is essential for:

• Proper trafficking of the receptor to the plasma membrane
• High-affinity CGRP binding
• Efficient signal transduction upon ligand binding

• CALCRL alone has low affinity for CGRP
• RAMP1 association enables high-affinity CGRP binding (Kd ~ 1-10 pM)
• RAMP1 also influences affinity for related peptides (αCGRP, βCGRP, amylin)

Pain and Migraine

RAMP1 is central to migraine pathophysiology:

Trigeminal System: RAMP1 is highly expressed in trigeminal ganglion neurons that innervate meningeal blood vessels. Activation of CGRP receptors on these neurons triggers the migraine pain pathway.

Vasodilation: CGRP is the most potent vasodilator known. CGRP-induced vasodilation of meningeal and cerebral blood vessels is a key component of migraine pathophysiology.

Central Processing: RAMP1 is expressed in brain regions involved in pain processing, including the thalamus and trigeminal nucleus caudalis.

Sensitization: CGRP signaling through RAMP1 can cause peripheral and central sensitization, amplifying pain signals.

Neuroprotection

CGRP signaling through RAMP1 provides neuroprotective effects:

Ischemic Protection: CGRP is released during cerebral ischemia and provides protective effects through RAMP1:

• Reduction of infarct size
• Improvement of cerebral blood flow
• Anti-apoptotic effects
• Reduction of oxidative stress

Anti-inflammatory Effects: CGRP can modulate immune cell function, reducing neuroinflammation that contributes to neurodegeneration[@meng2019].

Cardiovascular Function

While not the focus of this page, RAMP1-mediated CGRP signaling affects:

• Systemic blood pressure regulation
• Cardiac function
• Peripheral circulation

Expression and Localization

Brain Regional Distribution

RAMP1 exhibits region-specific expression:

• Trigeminal Ganglion: Highest expression—primary site for migraine pain initiation
• Dorsal Root Ganglion: Sensory neurons involved in pain signaling
• Cerebral Cortex: Variable expression across layers
• Hippocampus: Detected in CA1 and dentate gyrus
• Thalamus: Pain processing regions
• Brainstem: Trigeminal nucleus caudalis

Cellular and Subcellular Localization

At the cellular level:

• Plasma Membrane: Primary localization in neuronal membranes
• Endoplasmic Reticulum: Site of receptor assembly
• Axonal Compartments: In neurons, transported to peripheral and central terminals
• Glial Cells: Some expression in astrocytes and microglia

Role in Migraine

Clinical Evidence

RAMP1 is directly implicated in migraine:

Expression: RAMP1 expression is elevated in trigeminal ganglion of migraine patients.

Genetic Studies: RAMP1 polymorphisms have been associated with migraine susceptibility in some populations.

Therapeutic Validation: The efficacy of CGRP receptor antagonists (gepants) and CGRP antibodies (erenumab, fremanezumab, galcanezumab, eptinezumab) confirms the importance of RAMP1-CGRP signaling in migraine.

Mechanisms in Migraine

CGRP-RAMP1 signaling contributes to migraine through:

Peripheral Activation: CGRP released from trigeminal nerve endings activates RAMP1-containing receptors on:

• Vascular endothelial cells (causing vasodilation)
• Perivascular nerve endings (sending pain signals)
• Immune cells (releasing inflammatory mediators)

Cortical Spreading Depression: Some evidence links CGRP to cortical spreading depression, the purported correlate of migraine aura.

Paratriginal Nucleus Activation: RAMP1 in the paratriginal nucleus may contribute to migraine autonomic features.

Therapeutic Targeting

RAMP1 is a major therapeutic target for migraine:

CGRP Receptor Antagonists (Gepants):

• Ubrogepant (Ubrelvy)
• Rimegepant (Nurtec ODT)
• Atogepant (Qulipta)
• Zavegepant (intranasal)
• Block the CGRP-binding site on RAMP1-CALCRL complex

• Erenumab (Aimovig): Monoclonal antibody against CALCRL/RAMP1
• Fremanezumab (Ajovy): Monoclonal antibody against CGRP
• Galcanezumab (Emgality): Monoclonal antibody against CGRP
• Eptinezumab (Vyepti): Monoclonal antibody against CGRP

• Under development—targeting RAMP1 specifically rather than the entire receptor complex

Role in Alzheimer's Disease

Evidence

CGRP-RAMP1 signaling has been studied in Alzheimer's disease:

Expression Changes: Some studies show altered CGRP and RAMP1 expression in AD brains.

Neuroprotection Potential: CGRP signaling through RAMP1 may protect against amyloid-beta toxicity.

Synaptic Function: CGRP modulates synaptic transmission; disrupted signaling may contribute to synaptic dysfunction.

Mechanisms

Aβ Interaction: Some evidence suggests CGRP can reduce Aβ toxicity and may influence Aβ metabolism.

Neuroinflammation: CGRP has immunomodulatory effects that could influence neuroinflammation in AD.

Calcium Homeostasis: CGRP signaling affects calcium levels, relevant to calcium dysregulation in AD.

Potential Protection: The neuroprotective effects of CGRP may be beneficial in AD, though data are limited[@schurman2020].

Role in Stroke and Ischemia

Evidence

RAMP1-mediated CGRP signaling is protective in stroke:

Endogenous Protection: CGRP is released during ischemia and provides neuroprotection.

Therapeutic Potential: Exogenous CGRP or CGRP analogs may reduce infarct size.

Mechanisms

Vasodilation: Improved cerebral blood flow in ischemic penumbra.

Anti-apoptotic: Activation of pro-survival signaling pathways.

Anti-inflammatory: Modulation of post-ischemic inflammation.

Anti-oxidant: Reduction of oxidative stress[@yuan2019].

Role in Parkinson's Disease

Evidence

Limited evidence suggests CGRP-RAMP1 involvement in PD:

Expression Changes: Some studies show altered CGRP levels in PD patients.

Neuroprotection: CGRP may protect dopaminergic neurons.

Motor Function: CGRP may influence motor control circuits.

However, data are much more limited than for migraine or stroke[@chen2022].

Interacting Partners

| Partner | Interaction Type | Functional Role |
|---------|-----------------|-----------------|
| CALCRL | Heterodimer formation | CGRP receptor complex |
| CALCR | Alternative receptor | Amylin receptor formation |
| CGRP (αCGRP, βCGRP) | Ligand binding | Receptor activation |
| Receptor activity-modifying proteins | Heterodimerization | Determines ligand specificity |
| β-arrestin | Signal transduction | G protein-independent signaling |
| GRK | Phosphorylation | Receptor desensitization |

Signaling Pathways

CGRP-RAMP1 activates multiple signaling cascades:

cAMP/PKA Pathway: Primary pathway activated by CGRP, leading to:

• Vasodilation
• Neuronal activation
• Gene transcription changes

• Cell survival
• Synaptic plasticity
• Pain sensitization

PLC/IP3 Pathway: Secondary signaling for:

• Calcium release
• Smooth muscle contraction

Animal Models

Ramp1 Knockout Mice

Phenotype: Ramp1⁻/⁻ mice show:

• Loss of CGRP receptor binding
• Impaired vasodilatory responses
• Reduced neurogenic inflammation
• Altered pain responses

Transgenic Overexpression

Ramp1 overexpression: Enhances CGRP receptor function and sensitivity.

Disease Models

Migraine models: RAMP1 expression correlates with migraine-like behaviors.

Stroke models: CGRP-RAMP1 signaling is protective.

Research Methods

Study of RAMP1 employs various approaches:

• Radioligand binding: Quantify CGRP receptor density
• cAMP assays: Measure receptor activation
• Immunohistochemistry: Localize RAMP1 in tissues
• Electrophysiology: Study neuronal responses
• Behavioral testing: Pain and migraine behaviors

Therapeutic Approaches

Current Therapies

Gepants (CGRP receptor antagonists):

• Ubrogepant, Rimegepant, Atogepant, Zavegepant
• Bind to the CGRP binding pocket of the RAMP1-CALCRL complex

• Target either CGRP or the receptor complex
• Erenumab targets CALCRL/RAMP1 directly

Emerging Strategies

RAMP1-specific modulators: Target RAMP1 rather than entire receptor.

Allosteric modulators: Bind at distinct sites to modulate receptor function.

Gene therapy: Approaches to modulate RAMP1 expression.

Challenges

• Balancing neuroprotection versus migraine pain
• Species differences in pharmacology
• Peripheral versus central effects
• Long-term safety of chronic modulation

Cross-Links

• [RAMP1 Gene](/genes/ramp1)
• [Calcitonin Receptor Protein](/proteins/calcitonin-receptor-protein)
• [CGRP Receptor Complex](/mechanisms/cgrp-receptor)
• [Migraine](/diseases/migraine)
• [Alzheimer's Disease](/diseases/alzheimers-disease)
• [Stroke](/diseases/stroke)
• [Pain Signaling](/mechanisms/pain-signaling)

See Also

• [CGRP and Migraine](/mechanisms/cgrp-migraine)
• [Neuropeptide Signaling](/mechanisms/neuropeptide-signaling)
• [Receptor Activity Modifying Proteins](/mechanisms/ramp-family)
• [Trigeminal Pain](/mechanisms/trigeminal-pain)
• [Neuroprotection](/mechanisms/neuroprotection)

External Links

• [UniProt: O60883](https://www.uniprot.org/uniprot/O60883)
• [AlphaFold: O60883](https://alphafold.ebi.ac.uk/entry/O60883)
• [GeneCards: RAMP1](https://www.genecards.org/cgi-bin/carddisp.pl?gene=RAMP1)
• [OMIM: 604332](https://omim.org/entry/604332)

References