Mutagenetix > Incidental Mutation

Incidental Mutation 'R4788:Lgmn'

367270

Institutional Source

Beutler Lab

Gene Symbol

Lgmn

Ensembl Gene

ENSMUSG00000021190

Gene Name

legumain

Synonyms

Prsc1, preprolegumain, AEP

Accession Numbers

Essential gene?

Non essential (E-score: 0.000) question?

Stock #

R4788 (G1)

Quality Score

225

Status

Not validated

Chromosome

Chromosomal Location

102394084-102439813 bp(-) (GRCm38)

Type of Mutation

missense

DNA Base Change (assembly)

T to A at 102402677 bp (GRCm38)

Zygosity

Heterozygous

Amino Acid Change

Tyrosine to Phenylalanine at position 181 (Y181F)

Ref Sequence

ENSEMBL: ENSMUSP00000105647 (fasta)

Gene Model

predicted gene model for transcript(s): [ENSMUST00000021607] [ENSMUST00000110020]

AlphaFold

O89017

Predicted Effect

probably benign
Transcript: ENSMUST00000021607
AA Change: Y181F

PolyPhen 2 Score 0.106 (Sensitivity: 0.93; Specificity: 0.86)

SMART Domains

Protein: ENSMUSP00000021607
Gene: ENSMUSG00000021190
AA Change: Y181F

Domain	Start	End	E-Value	Type
low complexity region	5	22	N/A	INTRINSIC
Pfam:Peptidase_C13	31	288	8e-120	PFAM

Predicted Effect

probably benign
Transcript: ENSMUST00000110020
AA Change: Y181F

PolyPhen 2 Score 0.106 (Sensitivity: 0.93; Specificity: 0.86)

SMART Domains

Protein: ENSMUSP00000105647
Gene: ENSMUSG00000021190
AA Change: Y181F

Domain	Start	End	E-Value	Type
low complexity region	5	22	N/A	INTRINSIC
Pfam:Peptidase_C13	31	288	8e-120	PFAM

Predicted Effect

noncoding transcript
Transcript: ENSMUST00000146499

Coding Region Coverage

1x: 98.8%
3x: 98.4%
10x: 96.9%
20x: 94.4%

Validation Efficiency

MGI Phenotype

FUNCTION: This gene encodes a member of the cysteine peptidase family C13 that plays an important role in the endosome/lysosomal degradation system. The encoded inactive preproprotein undergoes autocatalytic removal of the C-terminal inhibitory propeptide to generate the active endopeptidase that cleaves protein substrates on the C-terminal side of asparagine residues. Mice lacking the encoded protein exhibit defects in the lysosomal processing of proteins resulting in their accumulation in the lysosomes, and develop symptoms resembling hemophagocytic lymphohistiocytosis. [provided by RefSeq, Aug 2016]
PHENOTYPE: Homozygotes for a null allele exhibit slow postnatal weight gain, develop features of hemophagocytic syndrome, and accumulate giant lysosomes in renal tubule cells. Homozygotes for another null allele display impaired TLR9 signaling in dendritic cells, progressive kidney pathology, and proteinuria. [provided by MGI curators]

Allele List at MGI

Other mutations in this stock

Total: 68 list
Gene	Ref	Var	Chr/Loc	Mutation	Predicted Effect	Zygosity
2010300C02Rik	A	T	1: 37,631,475	I128K	probably damaging	Het
Abca4	G	A	3: 122,166,712	D815N	probably damaging	Het
Abcc9	A	T	6: 142,620,730	C1135*	probably null	Het
Ap3b1	G	A	13: 94,565,641	M1067I	unknown	Het
Arhgap15	T	C	2: 43,748,890	M1T	probably null	Het
Boc	T	C	16: 44,500,433	D288G	probably damaging	Het
Brsk1	G	T	7: 4,698,955		probably null	Het
Cabp1	T	C	5: 115,175,471	N226S	probably benign	Het
Capn13	A	T	17: 73,337,432	Y367*	probably null	Het
Ccdc191	A	G	16: 43,956,822	E632G	probably damaging	Het
Cit	T	C	5: 115,933,506	S591P	probably damaging	Het
Ckmt1	T	C	2: 121,359,946	V118A	possibly damaging	Het
Cndp2	T	C	18: 84,675,164	N157S	probably damaging	Het
Col6a3	A	G	1: 90,772,950		probably null	Het
Coq2	A	T	5: 100,657,909	V287E	probably damaging	Het
Cpa6	T	C	1: 10,408,277	K278R	possibly damaging	Het
Cybb	C	G	X: 9,450,750	D246H	probably benign	Het
Cyp3a25	A	T	5: 145,985,082	Y347*	probably null	Het
Dcun1d4	G	T	5: 73,534,628	W160L	probably damaging	Het
Dennd4c	A	G	4: 86,819,963	T994A	probably benign	Het
Dhx57	T	C	17: 80,275,331	T229A	probably benign	Het
Dnah6	T	A	6: 73,129,530	R1741S	probably damaging	Het
Dock1	T	A	7: 135,145,484	V1508D	probably damaging	Het
Donson	T	C	16: 91,687,833	T117A	possibly damaging	Het
Dtnb	A	G	12: 3,772,699	D533G	probably damaging	Het
Fcrl5	A	G	3: 87,457,188	N470S	probably damaging	Het
Focad	T	A	4: 88,357,469	V1105E	unknown	Het
Fry	T	C	5: 150,399,636	V1084A	probably benign	Het
Gabra1	G	T	11: 42,147,153	R213S	probably damaging	Het
Gbp2b	A	C	3: 142,611,410	K509T	probably benign	Het
Gprc6a	T	C	10: 51,615,008	T811A	probably benign	Het
Hmgcs2	A	G	3: 98,291,084	D101G	probably damaging	Het
Ifna11	G	A	4: 88,820,008	W17*	probably null	Het
Ighv1-62-3	T	A	12: 115,461,052	M100L	probably benign	Het
Map4k4	T	C	1: 40,003,916	S644P	probably benign	Het
Med9	T	A	11: 59,948,440	N58K	probably benign	Het
Nav1	C	T	1: 135,469,723	A903T	probably benign	Het
Nop53	T	C	7: 15,942,315	E153G	possibly damaging	Het
Nop56	G	T	2: 130,278,900	V190L	probably benign	Het
Nyap2	A	T	1: 81,269,397	M687L	probably benign	Het
Olfr1254	G	A	2: 89,789,136	S72F	probably damaging	Het
Olfr146	T	C	9: 39,018,921	T207A	probably benign	Het
Olfr943	A	G	9: 39,184,612	T145A	probably benign	Het
Osbp2	T	C	11: 3,863,320	K183R	probably benign	Het
Pappa2	A	G	1: 158,783,917	V1492A	possibly damaging	Het
Pax1	A	G	2: 147,366,204	Q244R	possibly damaging	Het
Pcdh9	C	A	14: 93,887,415	V317F	probably damaging	Het
Pkhd1l1	A	T	15: 44,498,021	Q489L	probably damaging	Het
Poln	A	T	5: 34,129,331	S164R	probably benign	Het
Ptf1a	T	C	2: 19,445,951	S31P	probably benign	Het
Rasal3	A	T	17: 32,399,338	D164E	probably benign	Het
Rnf170	A	G	8: 26,140,863	E168G	probably damaging	Het
Rubcn	A	G	16: 32,836,408		probably null	Het
Sec16b	A	T	1: 157,561,524	T830S	possibly damaging	Het
Sel1l3	A	G	5: 53,131,833	V882A	probably benign	Het
Sfpq	A	G	4: 127,025,998	E512G	probably damaging	Het
Sh3pxd2a	A	G	19: 47,314,079	L187P	probably damaging	Het
Skint6	C	T	4: 113,238,336	G42D	possibly damaging	Het
Slc7a2	A	G	8: 40,913,986	I526V	probably benign	Het
Spata48	T	C	11: 11,488,652		probably null	Het
Ssh2	A	T	11: 77,429,798	N328Y	probably damaging	Het
Taok2	G	A	7: 126,868,132	S167L	possibly damaging	Het
Tcrg-V5	A	G	13: 19,192,554	K57R	probably benign	Het
Tom1l2	A	G	11: 60,249,018	L275P	probably damaging	Het
Tyrp1	C	T	4: 80,844,943	R356*	probably null	Het
Zan	A	G	5: 137,442,113	L1953P	unknown	Het
Zfhx3	T	C	8: 108,794,210	S655P	probably damaging	Het
Zmym1	T	C	4: 127,054,297	T94A	probably benign	Het

Other mutations in Lgmn

Allele	Source	Chr	Coord	Type	Predicted Effect	PPH Score
IGL00823:Lgmn	APN	12	102398176	splice site	probably benign
IGL02069:Lgmn	APN	12	102404299	missense	possibly damaging	0.92
IGL02150:Lgmn	APN	12	102395727	missense	possibly damaging	0.80
IGL02228:Lgmn	APN	12	102395714	missense	probably benign	0.04
IGL02637:Lgmn	APN	12	102400226	missense	probably damaging	0.98
Getz	UTSW	12	102399989	missense	probably damaging	0.99
R0233:Lgmn	UTSW	12	102399989	missense	probably damaging	0.99
R0233:Lgmn	UTSW	12	102399989	missense	probably damaging	0.99
R0988:Lgmn	UTSW	12	102398277	missense	probably damaging	0.99
R1451:Lgmn	UTSW	12	102405892	splice site	probably benign
R1568:Lgmn	UTSW	12	102394609	missense	possibly damaging	0.95
R1944:Lgmn	UTSW	12	102401924	missense	probably damaging	1.00
R1972:Lgmn	UTSW	12	102395821	unclassified	probably benign
R2133:Lgmn	UTSW	12	102394908	missense	probably damaging	1.00
R2298:Lgmn	UTSW	12	102395678	missense	probably damaging	0.99
R3846:Lgmn	UTSW	12	102404329	missense	possibly damaging	0.87
R4610:Lgmn	UTSW	12	102400124	splice site	probably benign
R5050:Lgmn	UTSW	12	102403421	splice site	probably null
R5708:Lgmn	UTSW	12	102404328	missense	possibly damaging	0.87
R5969:Lgmn	UTSW	12	102405827	missense	probably damaging	1.00
R6090:Lgmn	UTSW	12	102400154	missense	probably damaging	1.00
R6420:Lgmn	UTSW	12	102423719	nonsense	probably null
R6496:Lgmn	UTSW	12	102398239	missense	probably benign	0.01
R6592:Lgmn	UTSW	12	102404270	missense	probably damaging	1.00
R6659:Lgmn	UTSW	12	102402692	missense	probably benign	0.03
R7063:Lgmn	UTSW	12	102402678	missense	probably damaging	1.00
R7336:Lgmn	UTSW	12	102423739	start gained	probably benign

Predicted Primers

PCR Primer
(F):5'- AGGTACAGTGAATCCTGGGAC -3'
(R):5'- AGCTGTGCATGGAGAAGTGTC -3'

Sequencing Primer
(F):5'- AGTGAATCCTGGGACACCACTG -3'
(R):5'- GGCCAAGATGACATCTAGATTTTAC -3'

Posted On

2015-12-29