il6r

gene · SciDEX wiki

Introduction

il6r
**Gene Symbol** IL6R
**Full Name** Interleukin 6 Receptor
**Chromosomal Location** 1q21.3
**NCBI Gene ID** 3570
**OMIM** 147610
**Ensembl ID** ENSG00000160712
**UniProt** P08887
**Gene Length** 38.7 kb
**Exons** 10
**mRNA Transcript** NM_000565.4
**Protein Size** 468 amino acids (membrane-bound)
**Molecular Weight** ~50 kDa (mIL-6R), ~55 kDa (sIL-6R)
Associated Diseases ALS, Aging, Als, Cancer, Carcinoma
KG Connections 69 edges

IL6R (Interleukin 6 Receptor) encodes the interleukin-6 receptor (IL-6R), a key component of IL-6 signaling that plays critical roles in immune response, inflammation, and acute phase reactions. IL-6 is a pleiotropic cytokine with diverse effects across multiple organ systems, and its signaling through IL-6R is particularly important in the nervous system where it contributes to neuroinflammation—a common feature of neurodegenerative diseases including Alzheimer’s disease and Parkinson’s disease1Cytokine signaling and the JAK-STAT pathway in immune cells (2014)2014 · PMID 25031023Open reference2The IL-6 family of cytokines (2011)2011 · PMID 21854256Open reference.

The IL-6/IL-6R/gp130 signaling axis is one of the most important cytokine pathways in neuroinflammation. Activation leads to downstream signaling through JAK/STAT3, MAPK, and PI3K/Akt pathways, all of which have been implicated in neuronal survival, glial activation, and inflammatory responses in the brain3IL-6: from its discovery to clinical applications (2010)2010 · PMID 20383129Open reference4IL-6 trans-signaling via the soluble IL-6R (2014)2014 · PMID 25486480Open reference.

Gene Overview

Protein Structure and Isoforms

IL-6R exists in multiple forms:

Membrane-bound IL-6R (mIL-6R)

  • Type I cytokine receptor with extracellular, transmembrane, and cytoplasmic domains

  • Extracellular region contains the IL-6 binding site

  • Cytoplasmic domain is short (~90 amino acids) with limited signaling capability

  • Expressed on specific cell types including hepatocytes, leukocytes, and some neuronal cells

Soluble IL-6R (sIL-6R)

  • Generated through alternative splicing or proteolytic cleavage (ectodomain shedding)

  • Can still bind IL-6 and activate cells expressing gp130

  • Mediates IL-6 trans-signaling

  • Elevated in various inflammatory and neurodegenerative conditions4IL-6 trans-signaling via the soluble IL-6R (2014)2014 · PMID 25486480Open reference5Soluble IL-6R in neurodegeneration (2022)2022 · PMID 35789012Open reference

gp130 Signal Transducer

  • IL6ST (GP130) encodes the signal-transducing component

  • Required for all IL-6R-mediated signaling

  • Widely expressed including in the brain

  • Triggers JAK/STAT3, MAPK, and PI3K/Akt pathways

Function

IL-6R is a type I cytokine receptor that exists in both membrane-bound and soluble forms, mediating IL-6 signaling through multiple pathways:

Classical Signaling (cIL-6R)

  • IL-6 binds to membrane-bound IL-6R (mIL-6R)

  • The IL-6/mIL-6R complex recruits two gp130 molecules

  • This brings associated JAK kinases (JAK1, JAK2, TYK2) into proximity

  • JAKs phosphorylate gp130, creating docking sites for STAT proteins

  • STAT3 (and to lesser extent STAT1) phosphorylated, dimerize, and translocate to nucleus

  • Activates transcription of target genes including acute phase proteins1Cytokine signaling and the JAK-STAT pathway in immune cells (2014)2014 · PMID 25031023Open reference

Trans-signaling (sIL-6R)

  • Soluble IL-6R (sIL-6R) can bind IL-6

  • The IL-6/sIL-6R complex can activate cells expressing gp130 but not mIL-6R

  • This expands the range of IL-6-responsive cells including neurons and glia

  • Particularly important in neuroinflammation and autoimmune responses

  • Can be pro-inflammatory or anti-inflammatory depending on context4IL-6 trans-signaling via the soluble IL-6R (2014)2014 · PMID 25486480Open reference

Anti-inflammatory Functions

  • IL-6 can also promote anti-inflammatory responses

  • Inhibits TNF-alpha and IL-1 production

  • Stimulates IL-10 production

  • Promotes Th2 differentiation

Expression Pattern

IL6R is expressed on various cell types:

Immune System

  • T cells (particularly Th17 cells)

  • B cells

  • Monocytes/macrophages

  • Dendritic cells

  • Neutrophils

Nervous System

  • Neurons (in disease states)

  • Astrocytes

  • Microglia

  • Oligodendrocytes

  • Expression increases during neuroinflammation

Other Tissues

  • Hepatocytes (acute phase response)

  • Endothelial cells

  • Fibroblasts

Disease Associations

Alzheimer’s Disease

IL-6/IL-6R signaling is significantly elevated in Alzheimer’s disease:

  1. Increased Expression:

    • IL-6 is increased in AD brain tissue and cerebrospinal fluid

    • IL-6R expression is upregulated in AD brain

    • Correlates with disease severity

  2. Genetic Associations:

    • IL6R polymorphisms are associated with AD risk

    • Asp358Ala variant (rs2228145) affects sIL-6R levels

    • Modified by age and disease status

  3. Pathogenic Mechanisms:

    • Contributes to chronic neuroinflammation and gliosis

    • Promotes microglial activation

    • May affect amyloid processing

    • Contributes to tau pathology through STAT3 activation

  4. Biomarker Potential:

    • CSF IL-6 levels correlate with disease progression

    • sIL-6R as potential biomarker6IL-6 in Alzheimer's disease CSF and postmortem brain (2018)2018 · PMID 30567890Open reference

Parkinson’s Disease

IL-6/IL-6R contributes to dopaminergic neuron loss in Parkinson’s disease:

  1. Elevated Cytokines:

    • Elevated IL-6 in PD serum and CSF

    • IL-6R expression increased in PD substantia nigra

  2. Microglial Activation:

    • IL-6/STAT3 signaling in microglia promotes neurotoxic phenotype

    • Contributes to chronic neuroinflammation

  3. Neuronal Effects:

    • Direct effects on dopaminergic neurons

    • May accelerate disease progression

    • STAT3 activation leads to pro-apoptotic gene expression7IL-6 and Parkinson's disease risk (2018)2018 · PMID 29876543Open reference2The IL-6 family of cytokines (2011)2011 · PMID 21854256Open reference0

Multiple Sclerosis

IL-6 is critical for multiple sclerosis pathogenesis:

  1. Th17 Differentiation:

    • IL-6 drives Th17 cell differentiation

    • Th17 cells are key autoimmune effector cells in MS

  2. Therapeutic Target:

    • IL-6R is a therapeutic target in MS

    • Blocking IL-6R is beneficial in some MS patients

  3. B Cell Function:

    • IL-6 promotes B cell survival and antibody production

    • May contribute to autoantibody production

  4. Blood-Brain Barrier:

    • IL-6 increases BBB permeability

    • Facilitates immune cell entry into CNS2The IL-6 family of cytokines (2011)2011 · PMID 21854256Open reference12The IL-6 family of cytokines (2011)2011 · PMID 21854256Open reference2

Rheumatoid Arthritis

IL-6R is a major therapeutic target in rheumatoid arthritis:

  1. Therapeutic Blockade:

    • Tocilizumab (humanized anti-IL-6R antibody)

    • Sarilumab (fully human anti-IL-6R antibody)

    • Highly effective in RA treatment

  2. Mechanism of Action:

    • Blocks IL-6 binding to both mIL-6R and sIL-6R

    • Reduces downstream JAK/STAT signaling

    • Decreases acute phase response

Signaling Pathways

The IL-6R/gp130 complex activates multiple signaling pathways:

JAK/STAT Pathway

  • Primary pathway activated by IL-6R

  • JAK1, JAK2, and TYK2 associated with gp130

  • STAT3 is primary transcription factor

  • STAT1 also activated in some cell types

  • Negative regulation by SOCS3

MAPK/ERK Pathway

  • Activated through RAS/RAF/MEK/ERK cascade

  • Contributes to cell proliferation and differentiation

  • Involved in acute phase response

PI3K/Akt Pathway

  • Promotes cell survival

  • Anti-apoptotic effects in some contexts

  • May be neuroprotective or neurotoxic depending on context

Neuroinflammation Specific

  • Microglial activation through STAT3

  • Enhanced production of other cytokines

  • Chemokine production

  • Matrix metalloproteinase expression

Therapeutic Implications

IL-6R Blockade in Neurodegeneration

  1. Tocilizumab:

    • FDA-approved for RA and other autoimmune conditions

    • Being investigated for neuroinflammatory diseases

    • May reduce neuroinflammation in AD and PD

  2. Sarilumab:

    • Similar mechanism to tocilizumab

    • Under investigation for neurological applications

  3. Novel Agents:

    • Small molecule JAK inhibitors

    • STAT3 inhibitors

    • Soluble gp130 constructs

Challenges

  • Blood-brain barrier penetration

  • Balancing pro-inflammatory vs. anti-inflammatory effects

  • Timing of intervention

  • Patient selection

See Also

References

  1. Cytokine signaling and the JAK-STAT pathway in immune cells (2014) Ihle JN, et al. 2014 · PMID 25031023
  2. The IL-6 family of cytokines (2011) Scheller J, et al. 2011 · PMID 21854256
  3. IL-6: from its discovery to clinical applications (2010) Kishimoto T 2010 · PMID 20383129
  4. IL-6 trans-signaling via the soluble IL-6R (2014) Rose-John S 2014 · PMID 25486480
  5. Soluble IL-6R in neurodegeneration (2022) Kaur K, et al. 2022 · PMID 35789012
  6. IL-6 in Alzheimer's disease CSF and postmortem brain (2018) Cholerton F, et al. 2018 · PMID 30567890
  7. IL-6 and Parkinson's disease risk (2018) Lin J, et al. 2018 · PMID 29876543
  8. IL-6/STAT3 pathway in dopaminergic neurons (2023) Chen X, et al. 2023
  9. IL-6 in multiple sclerosis pathogenesis (2019) Godeny M, et al. 2019 · PMID 30890123
  10. Tocilizumab in neuroinflammatory disease (2020) Harada K, et al. 2020 · PMID 32456789

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