icon_0328_cc_gen_hmr_bacteria-s

Gap Junctions Signaling

Gap junctions are specialized channels that facilitate the rapid transfer of molecules from one cell to another, allowing for direct communication between neighboring cells. This enables tissues to coordinate physiological responses with precision, making gap junctions essential for electrical and metabolic coupling in a wide variety of organs.

Gap Junction Signaling

Pathway Summary

Gap junction channels span two plasma membranes and are formed by the alignment of two hemichannels, each consisting of an oligomer of structural subunit proteins called Connexins (Cx). These junctional proteins constitute a multigene family whose members are distinguished according to their predicted molecular weight. A connexin structure consists of two extracellular loops, four membrane-spanning domains, one cytoplasmic loop, one N-terminal tail, and one C-terminal tail. During intercellular channel formation, six connexins oligomerize into a connexon or hemichannel that docks in homotypic, heterotypic and combined heterotypic/heteromeric arrangements. In total, as many as 14 different connexon arrangements can be formed when two members of the connexin family intermix. This is followed by connexon trafficking to the plasma membrane. The intact channel is formed when one hemichannel docks with a second in an opposing cell. Once assembled, groups of these intercellular channels (termed gap junctional plaques) mediate the passage of amino acids, second messengers, ions and other metabolites between the connected cytoplasmic domains.Connexin-43 is the most ubiquitously expressed of the connexins. It is endogenously expressed in at least 35 distinct tissues encompassing over 35 cell types that include cardiomyocytes, keratinocytes, astrocytes, endothelial cells and smooth-muscle cells among many others. It co-oligomerizes with other connexins such as Cx26 (keratinocytes and hepatocytes), Cx31 (keratinocytes and myocardium) and Cx46 (trans-Golgi network). However, it is unable to co-oligomerize with Cx32. Connexins also bind ZO-1 and ZO-2 at different stages of the cell cycle to regulate gap junction size and stability, interact directly with β-catenin to regulate gap-junctional intercellular cross-talk with WNT signaling (essential for cell survival), and regulate the turnover of Cx43-containing gap junctions, in turn stabilizing the junctions. The actin-binding protein Dbn-1 binds and links gap junctions to the sub-membrane cytoskeleton, whereas other cytoskeletal proteins such as Tubulin-α and β facilitate connexin-mediated transport.Consisting of hundreds of intercellular channels, gap junctions are critically important in regulating embryonic development, excitable cell contraction, tissue homeostasis, apoptosis, metabolic transport and normal cell growth and differentiation. GJ communication is controlled by neurotransmitters such as Norepinephrine, Dopamine, Serotonin and Glutamate, cytokines, growth factors, and other bioactive compounds such as lysophosphatidic acid. These biomolecules activate downstream kinases leading to increased levels of phosphorylation at specific sites and opening and closing of the channel. Kinases such as PKG, PKA, PKC and ERK1/2 play a role in phosphorylation and acute gating of gap junction channels. Gap junctional communication also gets disrupted in response to extracellular cues such as growth factors which regulate post-translational phosphorylation of Cx43 and connexin redirection from the plasma membrane.

Gap Junction Signaling Genes list

Explore Genes related to Gap Junction Signaling
ACTA1
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Human
actin alpha 1, skeletal muscle
ACTA2
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Human
actin alpha 2, smooth muscle
ACTB
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Human
actin beta
ACTC1
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Human
actin alpha cardiac muscle 1
ACTG1
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Human
actin gamma 1
ACTG2
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Human
actin gamma 2, smooth muscle
ADCY1
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Human
adenylate cyclase 1
ADCY10
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Human
adenylate cyclase 10
ADCY2
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Human
adenylate cyclase 2
ADCY3
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Human
adenylate cyclase 3
ADCY4
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Human
adenylate cyclase 4
ADCY5
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Human
adenylate cyclase 5
ADCY6
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Human
adenylate cyclase 6
ADCY7
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Human
adenylate cyclase 7
ADCY8
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Human
adenylate cyclase 8
ADCY9
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Human
adenylate cyclase 9
ADRB1
icon_0140_ls_gen_dna_rna-s
Human
adrenoceptor beta 1
AKT1
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Human
AKT serine/threonine kinase 1
AKT2
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Human
AKT serine/threonine kinase 2
AKT3
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Human
AKT serine/threonine kinase 3
BGLAP
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Human
bone gamma-carboxyglutamate protein
CAMP
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Human
cathelicidin antimicrobial peptide
CAV1
icon_0140_ls_gen_dna_rna-s
Human
caveolin 1
CCN3
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Human
cellular communication network factor 3
CSNK1A1
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Human
casein kinase 1 alpha 1
CSNK1D
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Human
casein kinase 1 delta
CSNK1E
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Human
casein kinase 1 epsilon
CSNK1G1
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Human
casein kinase 1 gamma 1
CSNK1G2
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Human
casein kinase 1 gamma 2
CSNK1G3
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Human
casein kinase 1 gamma 3
CTH
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Human
cystathionine gamma-lyase
CTNNB1
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Human
catenin beta 1
DBN1
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Human
drebrin 1
DRD1
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Human
dopamine receptor D1
DRD2
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Human
dopamine receptor D2
EGF
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Human
epidermal growth factor
EGFR
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Human
epidermal growth factor receptor
ERAS
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Human
ES cell expressed Ras
GAD1
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Human
glutamate decarboxylase 1
GAST
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Human
gastrin
GJA1
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Human
gap junction protein alpha 1
GJA10
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Human
gap junction protein alpha 10
GJA3
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Human
gap junction protein alpha 3
GJA4
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Human
gap junction protein alpha 4
GJA5
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Human
gap junction protein alpha 5
GJA8
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Human
gap junction protein alpha 8
GJA9
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Human
gap junction protein alpha 9
GJB1
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Human
gap junction protein beta 1
GJB2
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Human
gap junction protein beta 2
GJB3
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Human
gap junction protein beta 3
GJB6
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Human
gap junction protein beta 6
GJB7
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Human
gap junction protein beta 7
GJC1
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Human
gap junction protein gamma 1
GJC2
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Human
gap junction protein gamma 2
GJC3
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Human
gap junction protein gamma 3
GJD2
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Human
gap junction protein delta 2
GNAI1
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Human
G protein subunit alpha i1
GNAI2
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Human
G protein subunit alpha i2
GNAI3
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Human
G protein subunit alpha i3
GNAQ
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Human
G protein subunit alpha q
GNAS
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Human
GNAS complex locus
GRB2
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Human
growth factor receptor bound protein 2
GRIA1
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Human
glutamate ionotropic receptor AMPA type subunit 1
GRIA2
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Human
glutamate ionotropic receptor AMPA type subunit 2
GRIA3
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Human
glutamate ionotropic receptor AMPA type subunit 3
GRIA4
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Human
glutamate ionotropic receptor AMPA type subunit 4
GRIK1
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Human
glutamate ionotropic receptor kainate type subunit 1
GRIK2
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Human
glutamate ionotropic receptor kainate type subunit 2
GRIK3
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Human
glutamate ionotropic receptor kainate type subunit 3
GUCY1A1
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Human
guanylate cyclase 1 soluble subunit alpha 1
GUCY1A2
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Human
guanylate cyclase 1 soluble subunit alpha 2
GUCY1B1
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Human
guanylate cyclase 1 soluble subunit beta 1
GUCY1B2
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Human
guanylate cyclase 1 soluble subunit beta 2 (pseudogene)
GUCY2C
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Human
guanylate cyclase 2C
GUCY2D
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Human
guanylate cyclase 2D, retinal
GUCY2F
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Human
guanylate cyclase 2F, retinal
HRAS
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Human
HRas proto-oncogene, GTPase
HTR2A
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Human
5-hydroxytryptamine receptor 2A
HTR2B
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Human
5-hydroxytryptamine receptor 2B
HTR2C
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Human
5-hydroxytryptamine receptor 2C
ITPR1
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Human
inositol 1,4,5-trisphosphate receptor type 1
ITPR2
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Human
inositol 1,4,5-trisphosphate receptor type 2
ITPR3
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Human
inositol 1,4,5-trisphosphate receptor type 3
KRAS
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Human
KRAS proto-oncogene, GTPase
LPA
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Human
lipoprotein(a)
LPAR1
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Human
lysophosphatidic acid receptor 1
MAP2K1
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Human
mitogen-activated protein kinase kinase 1
MAP2K2
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Human
mitogen-activated protein kinase kinase 2
MAP2K5
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Human
mitogen-activated protein kinase kinase 5
MAP3K2
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Human
mitogen-activated protein kinase kinase kinase 2
MAPK1
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Human
mitogen-activated protein kinase 1
MAPK14
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Human
mitogen-activated protein kinase 14
MAPK3
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Human
mitogen-activated protein kinase 3
MAPK7
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Human
mitogen-activated protein kinase 7
MRAS
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Human
muscle RAS oncogene homolog
NOTUM
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Human
notum, palmitoleoyl-protein carboxylesterase
NPR1
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Human
natriuretic peptide receptor 1
NPR2
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Human
natriuretic peptide receptor 2
NPR3
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Human
natriuretic peptide receptor 3
NRAS
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Human
NRAS proto-oncogene, GTPase
NT5C
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Human
5', 3'-nucleotidase, cytosolic
OPN1SW
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Human
opsin 1, short wave sensitive
PDIA3
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Human
protein disulfide isomerase family A member 3
PIK3C2A
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Human
phosphatidylinositol-4-phosphate 3-kinase catalytic subunit type 2 alpha
PIK3C2B
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Human
phosphatidylinositol-4-phosphate 3-kinase catalytic subunit type 2 beta
PIK3C2G
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Human
phosphatidylinositol-4-phosphate 3-kinase catalytic subunit type 2 gamma
PIK3C3
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Human
phosphatidylinositol 3-kinase catalytic subunit type 3
PIK3CA
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Human
phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit alpha
PIK3CB
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Human
phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit beta
PIK3CD
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Human
phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit delta
PIK3CG
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Human
phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit gamma
PIK3R1
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Human
phosphoinositide-3-kinase regulatory subunit 1
PIK3R2
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Human
phosphoinositide-3-kinase regulatory subunit 2
PIK3R3
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Human
phosphoinositide-3-kinase regulatory subunit 3
PIK3R4
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Human
phosphoinositide-3-kinase regulatory subunit 4
PIK3R5
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Human
phosphoinositide-3-kinase regulatory subunit 5
PIK3R6
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Human
phosphoinositide-3-kinase regulatory subunit 6
PLCB1
icon_0140_ls_gen_dna_rna-s
Human
phospholipase C beta 1
PLCB2
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Human
phospholipase C beta 2
PLCB3
icon_0140_ls_gen_dna_rna-s
Human
phospholipase C beta 3
PLCB4
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Human
phospholipase C beta 4
PLCD1
icon_0140_ls_gen_dna_rna-s
Human
phospholipase C delta 1
PLCD3
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Human
phospholipase C delta 3
PLCD4
icon_0140_ls_gen_dna_rna-s
Human
phospholipase C delta 4
PLCE1
icon_0140_ls_gen_dna_rna-s
Human
phospholipase C epsilon 1
PLCG1
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Human
phospholipase C gamma 1
PLCG2
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Human
phospholipase C gamma 2
PLCH1
icon_0140_ls_gen_dna_rna-s
Human
phospholipase C eta 1
PLCH2
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Human
phospholipase C eta 2
PLCL1
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Human
phospholipase C like 1 (inactive)
PLCL2
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Human
phospholipase C like 2
PLCZ1
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Human
phospholipase C zeta 1
PPP3CA
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Human
protein phosphatase 3 catalytic subunit alpha
PPP3CB
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Human
protein phosphatase 3 catalytic subunit beta
PPP3CC
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Human
protein phosphatase 3 catalytic subunit gamma
PPP3R1
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Human
protein phosphatase 3 regulatory subunit B, alpha
PPP3R2
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Human
protein phosphatase 3 regulatory subunit B, beta
PRKACA
icon_0140_ls_gen_dna_rna-s
Human
protein kinase cAMP-activated catalytic subunit alpha
PRKACB
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Human
protein kinase cAMP-activated catalytic subunit beta
PRKACG
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Human
protein kinase cAMP-activated catalytic subunit gamma
PRKAG1
icon_0140_ls_gen_dna_rna-s
Human
protein kinase AMP-activated non-catalytic subunit gamma 1
PRKAG2
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Human
protein kinase AMP-activated non-catalytic subunit gamma 2
PRKAR1A
icon_0140_ls_gen_dna_rna-s
Human
protein kinase cAMP-dependent type I regulatory subunit alpha
PRKAR1B
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Human
protein kinase cAMP-dependent type I regulatory subunit beta
PRKAR2A
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Human
protein kinase cAMP-dependent type II regulatory subunit alpha
PRKAR2B
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Human
protein kinase cAMP-dependent type II regulatory subunit beta
PRKCA
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Human
protein kinase C alpha
PRKCB
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Human
protein kinase C beta
PRKCD
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Human
protein kinase C delta
PRKCE
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Human
protein kinase C epsilon
PRKCG
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Human
protein kinase C gamma
PRKCH
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Human
protein kinase C eta
PRKCI
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Human
protein kinase C iota
PRKCQ
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Human
protein kinase C theta
PRKCZ
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Human
protein kinase C zeta
PRKD1
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Human
protein kinase D1
PRKD3
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Human
protein kinase D3
PRKG1
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Human
protein kinase cGMP-dependent 1
PRKG2
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Human
protein kinase cGMP-dependent 2
RAF1
icon_0140_ls_gen_dna_rna-s
Human
Raf-1 proto-oncogene, serine/threonine kinase
RALA
icon_0140_ls_gen_dna_rna-s
Human
RAS like proto-oncogene A
RALB
icon_0140_ls_gen_dna_rna-s
Human
RAS like proto-oncogene B
RAP1A
icon_0140_ls_gen_dna_rna-s
Human
RAP1A, member of RAS oncogene family
RAP1B
icon_0140_ls_gen_dna_rna-s
Human
RAP1B, member of RAS oncogene family
RAP2A
icon_0140_ls_gen_dna_rna-s
Human
RAP2A, member of RAS oncogene family
RAP2B
icon_0140_ls_gen_dna_rna-s
Human
RAP2B, member of RAS oncogene family
RASD1
icon_0140_ls_gen_dna_rna-s
Human
ras related dexamethasone induced 1
RASD2
icon_0140_ls_gen_dna_rna-s
Human
RASD family member 2
RRAS
icon_0140_ls_gen_dna_rna-s
Human
RAS related
RRAS2
icon_0140_ls_gen_dna_rna-s
Human
RAS related 2
SGSM3
icon_0140_ls_gen_dna_rna-s
Human
small G protein signaling modulator 3
SLC39A7
icon_0140_ls_gen_dna_rna-s
Human
solute carrier family 39 member 7
SMARCC2
icon_0140_ls_gen_dna_rna-s
Human
SWI/SNF related, matrix associated, actin dependent regulator of chromatin subfamily c member 2
SOS1
icon_0140_ls_gen_dna_rna-s
Human
SOS Ras/Rac guanine nucleotide exchange factor 1
SOS2
icon_0140_ls_gen_dna_rna-s
Human
SOS Ras/Rho guanine nucleotide exchange factor 2
SOX15
icon_0140_ls_gen_dna_rna-s
Human
SRY-box transcription factor 15
SP1
icon_0140_ls_gen_dna_rna-s
Human
Sp1 transcription factor
SP3
icon_0140_ls_gen_dna_rna-s
Human
Sp3 transcription factor
SRC
icon_0140_ls_gen_dna_rna-s
Human
SRC proto-oncogene, non-receptor tyrosine kinase
TJP1
icon_0140_ls_gen_dna_rna-s
Human
tight junction protein 1
TJP2
icon_0140_ls_gen_dna_rna-s
Human
tight junction protein 2
TUBA1A
icon_0140_ls_gen_dna_rna-s
Human
tubulin alpha 1a
TUBA1B
icon_0140_ls_gen_dna_rna-s
Human
tubulin alpha 1b
TUBA1C
icon_0140_ls_gen_dna_rna-s
Human
tubulin alpha 1c
TUBA3E
icon_0140_ls_gen_dna_rna-s
Human
tubulin alpha 3e
TUBA4A
icon_0140_ls_gen_dna_rna-s
Human
tubulin alpha 4a
TUBA8
icon_0140_ls_gen_dna_rna-s
Human
tubulin alpha 8
TUBB
icon_0140_ls_gen_dna_rna-s
Human
tubulin beta class I
TUBB1
icon_0140_ls_gen_dna_rna-s
Human
tubulin beta 1 class VI
TUBB2A
icon_0140_ls_gen_dna_rna-s
Human
tubulin beta 2A class IIa
TUBB2B
icon_0140_ls_gen_dna_rna-s
Human
tubulin beta 2B class IIb
TUBB3
icon_0140_ls_gen_dna_rna-s
Human
tubulin beta 3 class III
TUBB4A
icon_0140_ls_gen_dna_rna-s
Human
tubulin beta 4A class IVa
TUBB4B
icon_0140_ls_gen_dna_rna-s
Human
tubulin beta 4B class IVb
TUBB6
icon_0140_ls_gen_dna_rna-s
Human
tubulin beta 6 class V
TUBB8
icon_0140_ls_gen_dna_rna-s
Human
tubulin beta 8 class VIII
TUBG1
icon_0140_ls_gen_dna_rna-s
Human
tubulin gamma 1

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Gap junctions - molecular structure and components

In vertebrates, gap junctions are hexameric intercellular channels formed by proteins of the connexin family. Six connexin subunits assemble into a hemichannel, or connexon, which docks with another connexon on an adjacent cell to create a continuous pore that bridges the cytoplasm of the two cells.

Connexon composition is highly variable. Channels may be homomeric, composed of a single connexin type, or heteromeric, containing a mix of different connexins. These combinations result in channels with distinct electrical conductance, gating properties and permeability profiles. Nearly all cell types express connexins, although the specific isoforms vary by tissue, giving rise to specialized channel functions.

Mechanism of gap junction signaling

Gap junction signaling follows a series of steps beginning with connexin biosynthesis followed by channel formation, culminating in the direct exchange of ions and small molecules between neighboring cells.

Connexin formation

Connexins are a family of tetraspan transmembrane proteins that form the basic building blocks of gap junction channels. Individual connexins are synthesized in the endoplasmic reticulum, where they undergo folding, quality control and oligomerization. Six connexin subunits assemble into a hemichannel, also known as a connexon, within the Golgi apparatus.

Channel formation

Once assembled, connexons are trafficked to the plasma membrane, where they insert as hemichannels. Functional intercellular channels form when a connexon in one cell docks with a connexon in an adjacent cell, aligning their central pores to create a continuous channel across the intercellular gap. Clusters of these channels aggregate into gap junction plaques, which can expand, shrink or remodel in response to cellular conditions. The gating of these channels is regulated by voltage, pH, phosphorylation and intracellular calcium levels, allowing cells to dynamically open or close communication pathways.

Molecular exchange

Through these channels, cells exchange many different small molecules, typically under 1 kDa in size. These molecules include inorganic ions such as potassium and calcium, metabolic intermediates like ATP and glucose-6-phosphate and signaling molecules such as cyclic AMP (cAMP) and inositol trisphosphate (IP3). The direct passage of these molecules enables cells to synchronize electrical activity, coordinate metabolic states and propagate second messenger signals rapidly across tissues. By bypassing extracellular receptors and diffusion through the interstitial space, gap junctions provide one of the most efficient means of intercellular signaling in multicellular organisms.

Regulation of gap junctions

Multiple signaling pathways dynamically regulate the assembly, gating and turnover of gap junctions. The mechanisms include:

  • Growth factor signaling
    Growth factors such as EGF and TGF-β activate intracellular signaling cascades that regulate connexin phosphorylation and trafficking in response to growth signals.
  • Phosphorylation and kinase signaling
    Connexins such as Cx43 are extensively regulated by phosphorylation. Kinases including PKC, CK1, MAPKs, and Src-family kinases phosphorylate connexin residues, which directly impacts channel opening, trafficking and degradation.
  • Calcium and pH sensitivity
    Intracellular calcium elevation or acidification closes gap junction channels, serving as a protective mechanism that isolates injured or stressed cells from their neighbors.
  • Voltage gating
    Connexin isoforms show different sensitivity to transjunctional voltage. Some connexins close in response to voltage gradients, while others remain open. These different responses help tailor electrical coupling to tissue-specific needs such as rapid conduction in cardiac muscle or synchronization in neurons.
  • Connexin turnover
    Connexins are highly dynamic proteins with half-lives of only a few hours. Gap junction plaques are removed from the plasma membrane through internalization into double-membrane vesicles called annular junctions, which are then targeted for lysosomal or proteasomal degradation. This turnover is tightly controlled by post-translational modifications such as ubiquitination and phosphorylation.

Gap junction biological functions

Gap junctions support a wide variety of biological functions that extend beyond simple molecular exchange, enabling cells to act in coordinated networks rather than as isolated units. Their roles span development, tissue repair, electrophysiological synchronization and mechanosensing.

Tissue development and regeneration

During embryonic development, gap junctions ensure coordinated differentiation and organ formation by facilitating the spread of morphogen signals and synchronizing gene expression patterns across groups of cells. Later in life, they remain essential for tissue repair, helping transmit calcium and ATP signals that direct cell migration and proliferation during wound healing and regeneration.

Electrophysiological signaling

Gap junctions enable rapid and coordinated signaling in excitable tissues. For example, within the nervous system, neuronal gap junctions form electrical synapses that synchronize activity across networks. In cardiac muscle, where the atrial and ventricular chambers need to contract coordinatedly, connexins such as Cx43 and Cx45 assemble into channels that provide low-resistance conduits for depolarizing currents.

Mechanical sensing

Gap junctions also function as mechanosensors that respond to physical forces. In endothelial and epithelial tissues, connexins detect changes in shear stress or stretch and relay these signals to neighboring cells through changes in calcium level and second messengers.

Bone homeostasis

In the skeletal system, gap junctions connect osteoblasts, osteoclasts and osteocytes into an integrated signaling network that regulates bone remodeling. Connexin 43 (Cx43) is particularly abundant in osteocytes, where it facilitates transmission of mechanical strain signals to bone-forming osteoblasts, helping to maintain skeletal integrity throughout an individual’s lifetime.

Clinical relevance of connexin dysfunction

Mutations in connexin genes are associated with a group of disorders oftentimes referred to as “channelopathies” or “communication-opathies”. For example, mutations in GJB2 (encoding connexin 26) which disrupt potassium levels and impair electrical signals in the cochlea are the most common cause of hereditary deafness.

Connexin mutations are also associated with neuropathies such as Charcot–Marie–Tooth disease, and in cardiac arrhythmias where disrupted gap junction signaling impairs conduction. Dysregulated connexin expression has additionally been observed in cancer, where altered intercellular communication influences tumor progression and metastasis.

Pharmacological modulators of connexins, including mimetic peptides and small molecules, are being explored as therapeutic agents for diseases linked to connexin dysfunction.

References

  1. Goodenough DA, Paul DL. Gap junctions. Cold Spring Harb Perspect Biol. 2009;1(1):a002576.
  2. Nielsen MS, Axelsen LN, Sorgen PL, Verma V, Delmar M, Holstein-Rathlou NH. Gap junctions. Compr Physiol. 2012;2(3):1981–2035.
  3. Laird DW. Life cycle of connexins in health and disease. Biochem J. 2006;394(Pt 3):527–543.