Congenital Hydrocephalus in Genetically Engineered Mice

@article{Vogel2012CongenitalHI,
  title={Congenital Hydrocephalus in Genetically Engineered Mice},
  author={Peter Vogel and Robert W Read and Gwenn M Hansen and Bobby Joe Payne and Daniel L Small and Arthur T. Sands and Brian Zambrowicz},
  journal={Veterinary Pathology},
  year={2012},
  volume={49},
  pages={166 - 181}
}
There is evidence that genetic factors play a role in the complex multifactorial pathogenesis of hydrocephalus. Identification of the genes involved in the development of this neurologic disorder in animal models may elucidate factors responsible for the excessive accumulation of cerebrospinal fluid in hydrocephalic humans. The authors report here a brief summary of findings from 12 lines of genetically engineered mice that presented with autosomal recessive congenital hydrocephalus. This study… 
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Strain-dependent brain defects in mouse models of primary ciliary dyskinesia with mutations in Pcdp1 and Spef2
The Genetic Basis of Hydrocephalus.
TLDR
This work synthesizes the currently implicated genes and inheritance paradigms underlying hydrocephalus, grouping causal loci into functional modules that affect discrete, albeit partially overlapping, cellular processes that have the potential to both inform pathomechanism and assist in the rational molecular classification of a clinically heterogeneous phenotype.
Histopathology is required to identify and characterize myopathies in high-throughput phenotype screening of genetically engineered mice
TLDR
The findings support the need to include histopathology in phenotype screening protocols in order to identify novel genetic myopathies that are not clinically evident or not detected by the inverted screen test.
NME5 frameshift variant in Alaskan Malamutes with primary ciliary dyskinesia
TLDR
NME5 is identified as a novel candidate gene for unsolved human PCD and/or hydrocephalus cases and proposed NME5:c.43delA as the most likely candidate causative variant for PCD in Alaskan Malamutes to avoid the unintentional breeding of affected dogs in the future.
Semi-Lethal Primary Ciliary Dyskinesia in Rats Lacking the Nme7 Gene
TLDR
The knock-out of the rat Nme7 gene resulted in a range of conditions consistent with the presentation of primary ciliary dyskinesia, supporting the previously implicated role of the centrosomally located NME7 gene in ciliogenesis and control of ciliary transport.
NME 5 frameshift variant in Alaskan Malamutes with primary ciliary dyskinesia
TLDR
NME5 is identified as a novel candidate gene for unsolved human PCD and/ or hydrocephalus cases in Alaskan Malamutes and its findings enable genetic testing to avoid the unintentional breeding of affected dogs in the future.
Genetics and mechanisms leading to human cortical malformations.
Riding the wave of ependymal cilia: Genetic susceptibility to hydrocephalus in primary ciliary dyskinesia
  • Lance Lee
  • Medicine, Biology
    Journal of neuroscience research
  • 2013
TLDR
Mouse models of primary ciliary dyskinesia reveal strain‐specific differences in the appearance and severity of hydrocephalus, indicating the presence of genetic modifiers segregating in inbred strains.
Abnormal development of NG2+PDGFRα+ neural progenitor cells leads to neonatal hydrocephalus in a ciliopathy mouse model
TLDR
It is found that hydrocephalus in this mouse model is caused by aberrant platelet-derived growth factor receptor α (PDGFR-α) signaling, resulting in increased apoptosis and impaired proliferation of chondroitin sulfate proteoglycan 4 (also known as neuron-glial antigen 2 or NG2)+PDG FR-α+ neural progenitors.
Conditional N-WASP knockout in mouse brain implicates actin cytoskeleton regulation in hydrocephalus pathology
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