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Category Symbol Source: HGNC EntrezGene Ensembl GeneCards RNA genes CroW21

GIFtS
-

OPRM1 Gene

protein-coding GIFtS: 67
GCID: GC06P154391

opioid receptor, mu 1

Explore 76 diseases affiliated with
OPRM1 via

MalaCards

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Human Malady Compendium

(According to ¹HGNC, ²Entrez Gene,
³UniProtKB/Swiss-Prot, ⁴UniProtKB/TrEMBL, ⁵OMIM, ⁶GeneLoc, ⁷Ensembl, ⁸DME, ⁹miRBase, and/or ¹⁰fRNAdb)
About This Section

Aliases
Opioid Receptor, Mu 1¹ ²		OPRM²
MOR1¹ ² ³		Mu Opioid Receptor HMOR-1a²
Mu Opiate Receptor² ³		Mu-Type Opioid Receptor²
M-OR-1² ³		MOR-1³
MOP² ³		HMOP¹
LMOR²		Mu Opioid Receptor³
MOR²

External Ids:	HGNC: 8156¹	Entrez Gene: 4988²	Ensembl: ENSG00000112038⁷	OMIM: 600018⁵	UniProtKB: P35372³

Export aliases for OPRM1 gene to outside databases

Previous GC identifers: GC06P153921 GC06P154255 GC06P154452 GC06P151895

(According to Entrez Gene, Tocris Bioscience, Wikipedia's Gene Wiki, PharmGKB,
UniProtKB/Swiss-Prot, and/or UniProtKB/TrEMBL)
About This Section

Entrez Gene summary for OPRM1:

This gene encodes one of three opioid receptors. The mu opioid receptor is the principal target of endogenous opioid

peptides and opioid analgesic agents such a s beta-endorphn and enkephalins. The NM_001008503.1:c.118A>G allele had

been associated with opioid and alcohol addiction and variations in pain sensitivity but evidence is conflicting.

Multiple transcript variants encoding different isoforms have been found for this gene. (provided by RefSeq, Jun 2012)

UniProtKB/Swiss-Prot: OPRM_HUMAN, P35372

Function: Receptor for endogenous opioids such as beta-endorphin and endomorphin. Receptor for natural and synthetic

opioids including morphine, heroin, DAMGO, fentanyl, etorphine, buprenorphin and methadone. Agonist binding to the

receptor induces coupling to an inactive GDP-bound heterotrimeric G-protein complex and subsequent exchange of GDP for

GTP in the G-protein alpha subunit leading to dissociation of the G-protein complex with the free GTP-bound G-protein

alpha and the G-protein beta-gamma dimer activating downstream cellular effectors. The agonist- and cell type-specific

activity is predominantly coupled to pertussis toxin-sensitive G(i) and G(o) G alpha proteins, GNAI1, GNAI2, GNAI3 and

GNAO1 isoforms Alpha-1 and Alpha-2, and to a lesser extend to pertussis toxin-insensitive G alpha proteins GNAZ and

GNA15. They mediate an array of downstream cellular responses, including inhibition of adenylate cyclase activity and

both N-type and L-type calcium channels, activation of inward rectifying potassium channels, mitogen-activated protein

kinase (MAPK), phospholipase C (PLC), phosphoinositide/protein kinase (PKC), phosphoinositide 3-kinase (PI3K) and

regulation of NF-kappa-B. Also couples to adenylate cyclase stimulatory G alpha proteins. The selective temporal

coupling to G-proteins and subsequent signaling can be regulated by RGSZ proteins, such as RGS9, RGS17 and RGS4.

Phosphorylation by members of the GPRK subfamily of Ser/Thr protein kinases and association with beta-arrestins is

involved in short-term receptor desensitization. Beta-arrestins associate with the GPRK-phosphorylated receptor and

uncouple it from the G-protein thus terminating signal transduction. The phosphorylated receptor is internalized

through endocytosis via clathrin-coated pits which involves beta-arrestins. The activation of the ERK pathway occurs

either in a G-protein-dependent or a beta-arrestin-dependent manner and is regulated by agonist-specific receptor

phosphorylation. Acts as a class A G-protein coupled receptor (GPCR) which dissociates from beta-arrestin at or near

the plasma membrane and undergoes rapid recycling. Receptor down-regulation pathways are varying with the agonist and

occur dependent or independent of G-protein coupling. Endogenous ligands induce rapid desensitization, endocytosis and

recycling whereas morphine induces only low desensitization and endocytosis. Heterooligomerization with other GPCRs

can modulate agonist binding, signaling and trafficking properties. Involved in neurogenesis. Isoform 12 couples to

GNAS and is proposed to be involved in excitatory effects. Isoform 16 and isoform 17 do not bind agonists but may act

through oligomerization with binding-competent OPRM1 isoforms and reduce their ligand binding activity

summary for OPRM1:

The mu opioid receptor, (also known as OP3, MOP, MOR), is a member of the opioid family of G-protein-coupled

receptors that also includes kappa, delta and NOP receptors. Three variants of the receptor designated mu1,

mu2 and mu3 have been characterized, arising from the alternative splicing of the this gene. mu Opioid

receptors are distributed throughout the neuraxis (neocortex, thalamus, nucleus accumbens, hippocampus,

amygdala) and in the peripheral nervous system (myenteric neurons and vas deferens). mu Opioid receptors

have been implicated in respiration, cardiovascular functions, feeding, learning and memory, intestinal

transit, locomotor activity, thermoregulation, hormone secretion and immune functions. The human gene

encoding the mu opioid receptor has been localized to chromosome 6 (6q24-q25).

Gene Wiki entry for OPRM1 (Mu Opioid receptor)

(According to GeneLoc and/or HGNC, and/or
Entrez Gene (NCBI build 37),
and/or miRBase,
Genomic Views according to UCSC (hg19) and Ensembl (release 69), Regulatory elements and Epigenetics data according to QIAGEN, SABiosciences, and/or SwitchGear Genomics)
About This Section

RefSeq DNA sequence:

NC_000006.11 NC_018917.1 NT_025741.15

Regulatory elements:

SABiosciences Regulatory transcription factor binding sites in the OPRM1 gene promoter:
NRSF form 1 NRSF form 2
Other transcription factors

SwitchGear Promoter luciferase reporter plasmid: OPRM1 promoter sequence

Search SABiosciences Chromatin IP Primers for OPRM1

Epigenetics:

QIAGEN PyroMark CpG Assay predesigned Pyrosequencing DNA Methylation assays in human, mouse, rat OPRM1

Genomic Location:
Genomic View: UCSC Golden Path with GeneCards custom track

Entrez Gene cytogenetic band: 6q24-q25 Ensembl cytogenetic band: 6q25.2 HGNC cytogenetic band: 6q24-q25

OPRM1 Gene in genomic location: bands according to Ensembl, locations according to (and/or Entrez Gene and/or Ensembl if different)
OPRM1 gene location

GeneLoc information about chromosome 6 GeneLoc Exon Structure

GeneLoc location for GC06P154391: view genomic region (about GC identifiers)

Start:	154,331,631 bp from pter	End:	154,568,001 bp from pter
Size:	236,371 bases	Orientation:	plus strand

(According to ¹UniProtKB, HORDE, neXtProt, Ensembl, and/or Reactome, Modification sites according to ²PhosphoSitePlus, Specific Peptides from DME, Protein expression images according to data from SPIRE MOPED and PaxDb, RefSeq according to NCBI, PDB rendering according to OCA and/or Proteopedia, Recombinant Proteins from EMD Millipore, R&D Systems, GenScript, Enzo Life Sciences, OriGene, Novus Biologicals, Sino Biological, ProSpec, and/or Uscn,
Biochemical Assays by EMD Millipore, R&D Systems, OriGene, GenScript, Cell Signaling Technology, Enzo Life Sciences, and/or Uscn, Ontologies according to Gene Ontology Consortium 01 Mar 2013 and Entrez Gene, Antibodies by EMD Millipore, R&D Systems, GenScript, Cell Signaling Technology, OriGene, Novus Biologicals, Thermo Fisher Scientific, Abcam, and/or Uscn)
About This Section

UniProtKB/Swiss-Prot: OPRM_HUMAN, P35372 (See protein sequence)

Recommended Name: Mu-type opioid receptor

Size: 400 amino acids; 44779 Da

Subunit: Forms homooligomers and heterooligomers with other GPCRs, such as OPRD1, OPRK1, OPRL1, NPFFR2, ADRA2A, SSTR2,

CNR1 and CCR5 (probably in dimeric forms). Interacts with PPL; the interaction disrupts agonist-mediated G-protein

activation. Interacts (via C-terminus) with DNAJB4 (via C-terminus). Interacts with calmodulin; the interaction

inhibits the constitutive activity of OPRM1; it abolishes basal and attenuates agonist-stimulated G-protein coupling.

Interacts with FLNA, PLD2, RANBP9 and WLS. Interacts with GPM6A, RTP4, SYP, GNAS, RGS9, RGS17, RGS20, RGS4, PPP1R9B

and HINT1 (By similarity)

Subcellular location: Cell membrane; Multi-pass membrane protein

Subcellular location: Isoform 12: Cytoplasm

Miscellaneous: OPRM1 is the main physiological target for most clinically important opioid analgesics. OPRM1-mediated

inhibition of voltage-gated calcium channels on central presynaptic terminals of primary afferent nociceptors is

thought to be one of the primary mechanisms mediating analgesia at the spinal level. Opioid-induced hyperalgesic

responses are observed following both acute and chronic dosing associated with cellular excitation

Sequence caution: Sequence=CAI20458.1; Type=Erroneous initiation; Sequence=EAW47705.1; Type=Erroneous initiation;

Secondary accessions: B0FXJ1 B2R9S7 B8Q1L7 B8Q1L8 B8Q1L9 G8XRH6 G8XRH8 Q12930 Q4VWM1 Q4VWM2 Q4VWM3

Q4VWM4 Q4VWM6 Q4VWX6 Q5TDA1 Q6UPP1 Q6UQ80 Q7Z2D8 Q86V80 Q8IWW3 Q8IWW4 Q9UCZ4 Q9UN57

Alternative splicing: 17 isoforms: P35372-1 P35372-2 P35372-3 P35372-4 P35372-5 P35372-6 P35372-7 P35372-8

P35372-9 P35372-10 P35372-11 P35372-12 P35372-13 P35372-14 P35372-15 P35372-16

P35372-17 (Ref.5 (AAQ77392) sequence differs from that shown due to a polymorphism leading to premature termination of translation (position: 411:Q->Stop))

Explore the universe of human proteins at neXtProt for OPRM1: NX_P35372

Post-translational modifications:

Phosphorylated. Differentially phosphorylated in basal and agonist-induced conditions. Agonist-mediated phosphorylation

modulates receptor internalization. Phosphorylated by ADRBK1 in a agonist-dependent manner. Phosphorylation at Tyr-168

requires receptor activation, is dependent on non-receptor protein tyrosine kinase Src and results in a decrease in

agonist efficacy by reducing G-protein coupling efficiency. Phosphorylated on tyrosine residues; the phosphorylation

is involved in agoinist-induced G-protein-indepenedent receptor down-regulation. Phosphorylation at Ser-377 is

involved in G-protein-dependent but not beta-arrestin-dependent activation of the ERK pathway (By similarity)¹

Ubiquitinated. A basal ubiquitination seems not to be related to degradation. Ubiquitination is increased upon

formation of OPRM1:OPRD1 oligomers leading to proteasomal degradation; the ubiquitination is diminished by RTP4 (By

similarity)¹

View modification sites using PhosphoSitePlus²

View neXtProt modification sites for NX_P35372

OPRM1 Protein expression data from MOPED and PaxDb: About this image

REFSEQ proteins (13 alternative transcripts):

NP_000905.3 NP_001008503.2 NP_001008504.2 NP_001008505.2 NP_001138751.1 NP_001138752.1 NP_001138753.1 NP_001138754.1

NP_001138755.1 NP_001138756.1 NP_001138757.1 NP_001138758.1 NP_001138759.1

ENSEMBL proteins:

ENSP00000430247 ENSP00000394624 ENSP00000430876 ENSP00000430260 ENSP00000328264

ENSP00000411903 ENSP00000410497 ENSP00000428018 ENSP00000430575 ENSP00000229768

ENSP00000403549 ENSP00000430097 ENSP00000431048 ENSP00000399359 ENSP00000413752

ENSP00000338381 ENSP00000429719 ENSP00000429373 ENSP00000353598

Reactome Protein details: P35372
Human Recombinant Protein Products:

	EMD Millipore Purified and/or Recombinant OPRM1 Protein
	Browse R&D Systems for human recombinant proteins
	Browse recombinant and purified proteins available from Enzo Life Sciences
	OriGene Purified Protein: OPRM1 OriGene Protein Over-expression Lysate (see all 6): OPRM1 OriGene Custom Protein Services for OPRM1
	GenScript Custom Purified and Recombinant Proteins Services for OPRM1
	Novus Biologicals OPRM1 Proteins Novus Biologicals OPRM1 Lysates
	Browse Sino Biological Recombinant Proteins
	Browse ProSpec Recombinant Proteins
	Browse Proteins at Uscn

Gene Ontology (GO): 5/6 cellular component terms (GO ID links to tree view) (see all 6): About this table

GO ID	Qualified GO term	Evidence	PubMed IDs
GO:0005624	membrane fraction	--	--
GO:0005783	endoplasmic reticulum	TAS	9242668
GO:0005794	Golgi apparatus	TAS	9242668
GO:0005886	plasma membrane	TAS	--
GO:0005887	integral to plasma membrane	TAS	7905839

OPRM1 for ontologies About GeneDecksing

OPRM1 Antibody Products:

	EMD Millipore Mono- and Polyclonal Antibodies for the study of OPRM1
	R&D Systems Antibodies for OPRM1 (mu Opioid R/OPMR1)
	Cell Signaling Technology (CST) Antibodies for OPRM1 (MOR-1)
	OriGene Antibodies: OPRM1 OriGene Custom Antibody Services for OPRM1
	GenScript Custom Superior Antibodies Services for OPRM1
	Novus Biologicals OPRM1 Antibodies
	Abcam antibodies for OPRM1
	Browse Antibodies at Uscn
	ThermoFisher Antibody for OPRM1

Assay Products for OPRM1:

	Browse Kits and Assays available from EMD Millipore
	OriGene Custom Immunoassay Development Browse OriGene Fluorogenic Cell Assay Kits
	Browse R&D Systems for biochemical assays
	GenScript OPRM1-overexpressing Cell Line for Assay
	Browse Enzo Life Sciences for kits & assays
	Browse ELISAs and CLIAs at Uscn

(According to InterPro, ProtoNet, UniProtKB, and/or BLOCKS, Sets of similar genes according to GeneDecks)
About This Section

OPRM1 for domains About GeneDecksing

4 InterPro domains/families:

IPR017452 GPCR_Rhodpsn_7TM

IPR001418 Opioid_rcpt

IPR000105 Mu_opioid_rcpt

IPR000276 GPCR_Rhodpsn

Graphical View of Domain Structure for InterPro Entry P35372

ProtoNet protein and cluster: P35372

2 Blocks protein families:

IPB000105 Mu opioid receptor signature

IPB001418 Opioid receptor signature

UniProtKB/Swiss-Prot: OPRM_HUMAN, P35372

Similarity: Belongs to the G-protein coupled receptor 1 family

(According to ¹UniProtKB, Genatlas, LifeMap Discovery™, IUBMB, and/or ²DME, Human phenotypes from GenomeRNAi, Animal models from MGI Mar 06 2013,
bound targets from SABiosciences, miRNA Gene Targets from miRTarBase shRNA from OriGene, RNAi from EMD Millipore, siRNAs from OriGene, QIAGEN, microRNA from QIAGEN, Gene Editing from DNA2.0, Clones from EMD Millipore, OriGene, SwitchGear Genomics, GenScript, Sino Biological, DNA2.0, and Vector BioLabs, Cell Lines from GenScript, LifeMap BioReagents, In Situ Hybridization Assays from Advanced Cell Diagnostics, Ontologies according to Gene Ontology Consortium 01 Mar 2013 via Entrez Gene.)
About This Section

Function Summary: