Mpdk5<CAST/Ei> QTL Variant Detail MGI Mouse (MGI:3603241)

Mpdk5^CAST/Ei
QTL Variant Detail

Summary

QTL variant:	Mpdk5^CAST/Ei
Name:	modifier of polycystic kidney disease 5; CAST/Ei
MGI ID:	MGI:3603241
QTL:	Mpdk5 Location: unknown Genetic Position: Chr2, Syntenic

Variant
origin

Strain of Specimen:

CAST/Ei

Variant
description

Allele Type:		QTL
Mutation:		Undefined
		This allele confers increased renal disease traits compared to C57BL/6J. (J:99468)
Inheritance:		Other (see notes)

Phenotypes

View phenotypes and curated references for all genotypes (concatenated display).

Notes

Mpdk5 exhibits additive inheritance.

Mapping and Phenotype information for this QTL, its variants and associated markers

J:99468

Linkage analysis was performed on 461 homozygous mutant animals from a (C57BL/6J-Cys1^cpk x CAST/Ei)F2 intercross to identify modifiers of the Cys1^cpk mutation. 79 microsatellite markers at an average spacing of 25 cM were used in the genome scan. C57BL/6J-Cys1^cpk mutant animals exhibit cystic kidney disease and biliary dysgenesis.

Major modifier loci mapped to 16 cM, 34 cM, and 54 cM on mouse Chromosome 4 in linkage to renal traits and biliary ductal expansion. These loci are named Mpdk1 (modifierof polycystic kidney disease 1), Mpdk2, and Mpdk3, respectively. Mpdk3 also shows linkage to cholangitis (LOD=4.8). CAST/Ei-derived alleles at Mpdk1, Mpdk2, and Mpdk3 confer increased renal traits (kidney length, weight, and volume) with a dominant mode of inheritance. Kif12 maps to the Mpdk2 region and is proposed as a candidate gene. The C57BL/6J allele of Kif12 has a 15 bp deletion corresponding to a 5 amino acid deletion in the predicted L2 loop of the kinesin molecular motor catalytic domain. In addition, the CAST/Ei Kif12 haplotype shows strong correlation with polycystic kidney disease severity in (C57BL/6J-Cys1^cpk x CAST/Ei)F2 mice.

Linkage to renal traits mapped to 26 cM on mouse Chromosome 1 with LOD=2.5. This locus is named Mpdk4 (modifier of polycystic kidney disease 4). CAST/Ei-derived alleles at Mpdk4 confer increased renal traits with an additive mode of inheritance.

Linkage to renal traits mapped to 8 cM on mouse Chromosome 2 with LOD=3.2. This locus is named Mpdk5 (modifier of polycystic kidney disease 5). CAST/Ei-derived alleles at Mpdk5 confer increased renal traits with an additive mode of inheritance.

Linkage to biliary ductal expansion mapped to 16 cM on mouse Chromosome 13 with LOD=6.8. This locus is named Mpdk6 (modifier ofpolycystic kidney disease 6) and exhibits overdominance.

Linkage to cholangitis mapped to 40 cM on mouse Chromosome 19 with LOD=2.7. This locus is named Mpdk7 (modifier of polycystic kidney disease 7). CAST/Ei-derived alleles at Mpdk7 confer increased cholangitis with an additive mode of inheritance.

Linkage to cholangitis mapped to 6 cM on mouse Chromosome 3 with LOD=3.3. This locus is named Mpdk8 (modifier of polycystic kidney disease 8). CAST/Ei-derived alleles at Mpdk8 confer increased cholangitis with an additive mode of inheritance.

Interaction between loci at 62 cM on mouse Chromosome 1 and 96 cM on mouse Chromosome 2 was detected for effects on biliary duct expansion. A second interacting locus pair affecting biliary duct expansionwas detected between 14 cM on mouse Chromosome 4 and 17 cM on mouse Chromosome 18.

References

Original:	J:99468 Mrug M, et al., Kinesin family member 12 is a candidate polycystic kidney disease modifier in the cpk mouse. J Am Soc Nephrol. 2005 Apr;16(4):905-16
All:	1 reference(s)

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