Mutagenetix > Incidental Mutation

Incidental Mutation 'IGL01338:Casp7'

74696

Institutional Source

Australian Phenomics Network (link to record)

Gene Symbol

Casp7

Ensembl Gene

ENSMUSG00000025076

Gene Name

caspase 7

Synonyms

ICE-IAP3, CMH-1, caspase-7, Mch3

Accession Numbers

Essential gene?

Non essential (E-score: 0.000) question?

Stock #

IGL01338

Quality Score

Status

Chromosome

Chromosomal Location

56385561-56430776 bp(+) (GRCm39)

Type of Mutation

missense

DNA Base Change (assembly)

T to C at 56392896 bp (GRCm39)

Zygosity

Heterozygous

Amino Acid Change

Serine to Proline at position 17 (S17P)

Ref Sequence

ENSEMBL: ENSMUSP00000026062 (fasta)

Gene Model

predicted gene model for transcript(s): [ENSMUST00000026062]

AlphaFold

P97864

Predicted Effect

probably benign
Transcript: ENSMUST00000026062
AA Change: S17P

PolyPhen 2 Score 0.000 (Sensitivity: 1.00; Specificity: 0.00)

SMART Domains

Protein: ENSMUSP00000026062
Gene: ENSMUSG00000025076
AA Change: S17P

Domain	Start	End	E-Value	Type
low complexity region	29	40	N/A	INTRINSIC
CASc	59	303	2.2e-135	SMART

Coding Region Coverage

Validation Efficiency

MGI Phenotype

FUNCTION: [Summary is not available for the mouse gene. This summary is for the human ortholog.] This gene encodes a member of the cysteine-aspartic acid protease (caspase) family. Sequential activation of caspases plays a central role in the execution-phase of cell apoptosis. Caspases exist as inactive proenzymes which undergo proteolytic processing at conserved aspartic residues to produce two subunits, large and small, that dimerize to form the active enzyme. The precursor of the encoded protein is cleaved by caspase 3 and 10, is activated upon cell death stimuli and induces apoptosis. Alternatively spliced transcript variants encoding multiple isoforms have been observed for this gene. [provided by RefSeq, May 2012]
PHENOTYPE: Mice homozygous for a targeted mutation have normal appearance, organ morphology and lymphoid development. [provided by MGI curators]

Allele List at MGI

Other mutations in this stock

Total: 48 list
Gene	Ref	Var	Chr/Loc	Mutation	Predicted Effect	Zygosity
Adam23	A	G	1: 63,591,014 (GRCm39)	T494A	possibly damaging	Het
Adamts16	C	T	13: 70,984,234 (GRCm39)	C143Y	probably damaging	Het
Cacna1i	A	G	15: 80,232,581 (GRCm39)	I195V	probably damaging	Het
Cfap298	T	C	16: 90,722,936 (GRCm39)	N266S	possibly damaging	Het
Cox6a1	C	A	5: 115,483,898 (GRCm39)		probably benign	Het
Cpvl	T	A	6: 53,951,640 (GRCm39)	S48C	possibly damaging	Het
Cyp2b19	G	T	7: 26,458,842 (GRCm39)	M138I	probably benign	Het
Dennd5a	T	C	7: 109,518,611 (GRCm39)	Y510C	possibly damaging	Het
Derl2	A	G	11: 70,901,181 (GRCm39)	F229S	possibly damaging	Het
Dlec1	A	G	9: 118,949,979 (GRCm39)	E452G	probably damaging	Het
Dsc2	T	C	18: 20,180,214 (GRCm39)	K180E	probably benign	Het
Dus1l	G	A	11: 120,683,918 (GRCm39)	R177C	possibly damaging	Het
Egfr	A	G	11: 16,813,020 (GRCm39)	I167V	probably damaging	Het
Fam219b	A	T	9: 57,445,305 (GRCm39)		probably null	Het
Fn1	T	C	1: 71,665,369 (GRCm39)	E916G	probably damaging	Het
Gm2058	C	T	7: 39,238,580 (GRCm39)		noncoding transcript	Het
Gpd1	T	A	15: 99,616,056 (GRCm39)	V22E	probably damaging	Het
Hsf2	T	C	10: 57,377,475 (GRCm39)	F124L	probably damaging	Het
I0C0044D17Rik	A	G	4: 98,708,336 (GRCm39)		probably benign	Het
Igfbp3	A	T	11: 7,158,478 (GRCm39)	F262I	possibly damaging	Het
Klhl18	A	G	9: 110,284,501 (GRCm39)	Y62H	probably damaging	Het
Lama2	C	T	10: 27,064,268 (GRCm39)	E1238K	probably benign	Het
Man1b1	A	G	2: 25,228,239 (GRCm39)	K170E	probably benign	Het
Mcrs1	A	T	15: 99,147,382 (GRCm39)	I39N	probably damaging	Het
Mug2	T	C	6: 122,026,587 (GRCm39)		probably benign	Het
Neu3	C	A	7: 99,462,629 (GRCm39)	G365W	probably damaging	Het
Nipal3	A	C	4: 135,199,194 (GRCm39)		probably null	Het
Nrxn3	A	G	12: 89,221,804 (GRCm39)	I528V	possibly damaging	Het
Or10al6	A	T	17: 38,082,730 (GRCm39)	H71L	possibly damaging	Het
Osbpl8	A	G	10: 111,103,608 (GRCm39)	K204R	probably damaging	Het
Pax8	A	G	2: 24,325,931 (GRCm39)	S318P	possibly damaging	Het
Pcdh18	T	A	3: 49,710,590 (GRCm39)	N242Y	probably damaging	Het
Pkd1l2	T	A	8: 117,786,259 (GRCm39)	K649*	probably null	Het
Ppm1n	A	T	7: 19,013,179 (GRCm39)	D257E	probably benign	Het
Pxdn	A	G	12: 30,052,796 (GRCm39)	E811G	probably damaging	Het
Relb	T	C	7: 19,350,298 (GRCm39)	I218V	probably benign	Het
Rreb1	T	C	13: 38,115,010 (GRCm39)	C790R	probably damaging	Het
Rtkn2	G	T	10: 67,861,349 (GRCm39)	C258F	possibly damaging	Het
Scn11a	G	A	9: 119,613,227 (GRCm39)		probably benign	Het
Snx8	G	A	5: 140,343,851 (GRCm39)	R96C	probably damaging	Het
Syne2	A	T	12: 76,107,000 (GRCm39)	T5649S	possibly damaging	Het
Tm2d3	T	A	7: 65,344,970 (GRCm39)	C82*	probably null	Het
Tnpo2	T	C	8: 85,767,155 (GRCm39)	L55P	probably damaging	Het
Tsc22d2	T	C	3: 58,324,836 (GRCm39)		probably benign	Het
Ttll3	T	G	6: 113,371,690 (GRCm39)	V19G	probably damaging	Het
Ube2r2	A	G	4: 41,174,119 (GRCm39)	I86V	probably benign	Het
Vps13d	G	A	4: 144,814,892 (GRCm39)	T3153I	probably damaging	Het
Wwp1	A	G	4: 19,627,636 (GRCm39)	I753T	probably damaging	Het

Other mutations in Casp7

Allele	Source	Chr	Coord	Type	Predicted Effect	PPH Score
IGL01109:Casp7	APN	19	56,425,177 (GRCm39)	missense	probably benign	0.00
IGL02831:Casp7	APN	19	56,392,855 (GRCm39)	missense	probably benign	0.01
IGL02886:Casp7	APN	19	56,421,775 (GRCm39)	missense	probably damaging	1.00
R1558:Casp7	UTSW	19	56,421,684 (GRCm39)	nonsense	probably null
R2026:Casp7	UTSW	19	56,424,830 (GRCm39)	missense	probably damaging	1.00
R5445:Casp7	UTSW	19	56,421,770 (GRCm39)	splice site	probably null
R5665:Casp7	UTSW	19	56,429,414 (GRCm39)	missense	probably benign	0.00
R5765:Casp7	UTSW	19	56,422,315 (GRCm39)	missense	possibly damaging	0.87
R6207:Casp7	UTSW	19	56,429,452 (GRCm39)	missense	possibly damaging	0.53
R6893:Casp7	UTSW	19	56,421,741 (GRCm39)	missense	probably damaging	1.00
R7261:Casp7	UTSW	19	56,424,765 (GRCm39)	missense	probably benign	0.00
R7271:Casp7	UTSW	19	56,424,793 (GRCm39)	missense	probably damaging	1.00
R8331:Casp7	UTSW	19	56,429,397 (GRCm39)	missense	probably damaging	1.00
R9498:Casp7	UTSW	19	56,424,767 (GRCm39)	missense	probably damaging	1.00

Posted On

2013-10-07