Mutagenetix > Incidental Mutation

Incidental Mutation 'IGL01018:Vip'

53816

Institutional Source

Australian Phenomics Network (link to record)

Gene Symbol

Vip

Ensembl Gene

ENSMUSG00000019772

Gene Name

vasoactive intestinal polypeptide

Synonyms

PHI, peptide histidine isoleucine

Accession Numbers

Essential gene?

Probably non essential (E-score: 0.177) question?

Stock #

IGL01018

Quality Score

Status

Chromosome

Chromosomal Location

5639218-5647617 bp(+) (GRCm38)

Type of Mutation

missense

DNA Base Change (assembly)

A to G at 5642480 bp (GRCm38)

Zygosity

Heterozygous

Amino Acid Change

Aspartic acid to Glycine at position 40 (D40G)

Ref Sequence

ENSEMBL: ENSMUSP00000019906 (fasta)

Gene Model

predicted gene model for transcript(s): [ENSMUST00000019906]

AlphaFold

no structure available at present

Predicted Effect

probably benign
Transcript: ENSMUST00000019906
AA Change: D40G

PolyPhen 2 Score 0.277 (Sensitivity: 0.91; Specificity: 0.88)

SMART Domains

Protein: ENSMUSP00000019906
Gene: ENSMUSG00000019772
AA Change: D40G

Domain	Start	End	E-Value	Type
signal peptide	1	25	N/A	INTRINSIC
GLUCA	82	108	2.87e-11	SMART
GLUCA	126	152	6.39e-9	SMART

Predicted Effect

noncoding transcript
Transcript: ENSMUST00000217331

Coding Region Coverage

Validation Efficiency

MGI Phenotype

FUNCTION: This gene encodes a neuropeptide of the glucagon/secretin superfamily with potent bronchodilator, immunomodulator and anti-inflammatory properties. The encoded protein is proteolytically processed to generate two structurally similar neuropeptides - vasoactive intestinal peptide (VIP) and peptide histidine isoleucine (PHI). In the digestive tract, VIP stimulates relaxation of enteric smooth muscle, secretion of water and electrolytes, release of insulin and glucagon, and inhibition of gastric acid secretion. In the cardiovascular system, VIP causes coronary vasodilation and stimulates contractility in the heart. Mice lacking VIP exhibit airway hyperresponsiveness and airway inflammation. Male mice lacking VIP exhibit moderate pulmonary arterial hypertension resulting in increased mortality. Alternative splicing results in multiple transcript variants encoding different isoforms. [provided by RefSeq, Sep 2015]
PHENOTYPE: Homozygous null mutants display abnormal circadian rhythyms with a shorter period, abnormal phase, and in 1/4 arrhythmic circadian persistence. [provided by MGI curators]

Allele List at MGI

Other mutations in this stock

Total: 51 list
Gene	Ref	Var	Chr/Loc	Mutation	Predicted Effect	Zygosity
4931408C20Rik	T	C	1: 26,682,910	E1063G	probably damaging	Het
5530400C23Rik	G	T	6: 133,294,497	R168I	probably benign	Het
5530400C23Rik	A	T	6: 133,294,498	R168S	probably benign	Het
9230019H11Rik	A	G	10: 3,120,231		noncoding transcript	Het
9230019H11Rik	A	G	10: 3,120,209		noncoding transcript	Het
9230019H11Rik	G	A	10: 3,125,031		noncoding transcript	Het
9230019H11Rik	C	T	10: 3,125,193		noncoding transcript	Het
Armt1	C	T	10: 4,454,237		probably benign	Het
Armt1	T	A	10: 4,450,732	S160T	probably benign	Het
Ccdc170	T	C	10: 4,512,788	W35R	probably benign	Het
Ccdc170	G	T	10: 4,514,155	A99S	probably benign	Het
Ccdc170	T	C	10: 4,514,114	V31A	probably benign	Het
Glp2r	C	A	11: 67,709,644	V460F	probably benign	Het
Gm21411	T	C	4: 146,892,577	Q80R	probably benign	Het
Gm21411	C	T	4: 146,892,610	S69N	possibly damaging	Het
Gm21671	G	T	5: 25,950,723	H208N	probably benign	Het
Gm21738	G	A	14: 19,418,856	P24L	probably benign	Het
H2-M10.6	C	T	17: 36,812,220	A15V	probably benign	Het
H60c	T	C	10: 3,259,766	M174V	probably benign	Het
H60c	A	C	10: 3,260,343	F69V	probably benign	Het
Ipcef1	C	T	10: 6,919,968	R144Q	probably damaging	Het
Ipcef1	G	A	10: 6,890,551	A382V	probably benign	Het
Mapk8ip3	T	G	17: 24,899,719		probably benign	Het
Mthfd1l	T	C	10: 4,032,345		probably benign	Het
Mthfd1l	T	C	10: 3,978,708	V100A	probably benign	Het
Mthfd1l	T	C	10: 4,007,800	V279A	probably benign	Het
Mtrf1l	A	G	10: 5,814,180		probably benign	Het
Myo18b	T	C	5: 112,809,747	E1450G	probably damaging	Het
Obscn	C	T	11: 59,128,069	V973M	probably damaging	Het
Olfr414	G	A	1: 174,431,342	V305I	probably benign	Het
Oprm1	T	C	10: 7,037,170		probably benign	Het
Pou5f2	A	G	13: 78,025,938		probably benign	Het
Ralgapa2	G	A	2: 146,410,193	H891Y	probably benign	Het
Ralgapa2	T	G	2: 146,410,192	H806P	probably benign	Het
Rmnd1	A	T	10: 4,427,290	S130T	probably benign	Het
Rmnd1	A	G	10: 4,427,392	W96R	probably benign	Het
Trappc12	A	C	12: 28,691,854		probably benign	Het
Vmn2r125	T	A	4: 156,351,226	L300M	probably benign	Het
Vmn2r125	T	C	4: 156,350,612		probably benign	Het
Vmn2r125	C	T	4: 156,351,038	T237I	probably benign	Het
Vmn2r125	A	T	4: 156,351,037	T237S	probably benign	Het
Vmn2r125	A	C	4: 156,350,900	Q191P	probably benign	Het
Vmn2r125	C	A	4: 156,350,899	Q191K	probably benign	Het
Vmn2r125	A	G	4: 156,350,845	N173D	probably damaging	Het
Vmn2r40	G	A	7: 8,908,176	S706F	probably damaging	Het
Vmn2r-ps159	A	T	4: 156,338,146		noncoding transcript	Het
Vmn2r-ps159	C	A	4: 156,338,435		noncoding transcript	Het
Vmn2r-ps159	T	C	4: 156,334,263		noncoding transcript	Het
Vmn2r-ps159	T	C	4: 156,335,590		noncoding transcript	Het
Vmn2r-ps159	G	A	4: 156,334,605		noncoding transcript	Het
Zfp14	T	A	7: 30,038,101	R486S	probably damaging	Het

Other mutations in Vip

Allele	Source	Chr	Coord	Type	Predicted Effect	PPH Score
IGL02182:Vip	APN	10	5643561	missense	probably benign	0.01
R0082:Vip	UTSW	10	5644953	makesense	probably null
R0267:Vip	UTSW	10	5644004	missense	possibly damaging	0.67
R1776:Vip	UTSW	10	5644992	critical splice donor site	probably null
R3973:Vip	UTSW	10	5642590	missense	possibly damaging	0.57
R4803:Vip	UTSW	10	5644099	missense	probably damaging	0.99
R5898:Vip	UTSW	10	5643988	missense	probably damaging	0.96
R6365:Vip	UTSW	10	5644021	nonsense	probably null
R9571:Vip	UTSW	10	5640661	missense	probably benign

Posted On

2013-06-28