Generation and characterisation of keratin 7 (K7) knockout mice

Keratin 7 (K7) is a Type II member of the keratin superfamily and despite its widespread expression in different types of simple and transitional epithelia, its functional role in vivo remains elusive, in part due to the lack of any appropriate mouse models or any human diseases that are associated...

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Bibliographic Details
Published in:PloS one 2013-05, Vol.8 (5), p.e64404-e64404
Main Authors: Sandilands, Aileen, Smith, Frances J D, Lunny, Declan P, Campbell, Linda E, Davidson, Kirsty M, MacCallum, Stephanie F, Corden, Laura D, Christie, Lesley, Fleming, Stewart, Lane, E Birgitte, McLean, W H Irwin
Format: Article
Language:English
Subjects:
Animal models
Animals
Biology
Bladder
Cell Proliferation
Dentistry
Dermatology
Embryo cells
Female
Founder Effect
Gene Expression Regulation
Gene targeting
Genes
Genotype & phenotype
Hepatitis
Hyperplasia
Immunofluorescence
Keratin
Keratin-18 - genetics
Keratin-18 - metabolism
Keratin-19 - genetics
Keratin-19 - metabolism
Keratin-20 - genetics
Keratin-20 - metabolism
Keratin-7 - deficiency
Keratin-7 - genetics
Keratin-8 - genetics
Keratin-8 - metabolism
Kidneys
Life sciences
Liver diseases
Male
Medical research
Medicine
Mice
Mice, Knockout - genetics
Mice, Knockout - metabolism
Microscopy
Monoclonal antibodies
Mutation
Protein Binding
Rodents
Stem cell transplantation
Stem cells
Transcription
Urinary bladder
Urinary Bladder - cytology
Urinary Bladder - metabolism
Urothelium
Urothelium - cytology
Urothelium - metabolism
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Summary:Keratin 7 (K7) is a Type II member of the keratin superfamily and despite its widespread expression in different types of simple and transitional epithelia, its functional role in vivo remains elusive, in part due to the lack of any appropriate mouse models or any human diseases that are associated with KRT7 gene mutations. Using conventional gene targeting in mouse embryonic stem cells, we report here the generation and characterisation of the first K7 knockout mouse. Loss of K7 led to increased proliferation of the bladder urothelium although this was not associated with hyperplasia. K18, a presumptive type I assembly partner for K7, showed reduced expression in the bladder whereas K20, a marker of the terminally differentiated superficial urothelial cells was transcriptionally up-regulated. No other epithelia were seen to be adversely affected by the loss of K7 and western blot and immunofluorescence microscopy analysis revealed that the expression of K8, K18, K19 and K20 were not altered in the absence of K7, with the exception of the kidney where there was reduced K18 expression.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0064404