Publication detail

Cdk13-/- Mice Exhibit Developmental Delay and Craniofacial Malformations during Embryonic Development

HAMPL, M. KAVKOVÁ, M. ZIKMUND, T. KAISER, J. BUCHTOVÁ, M.

Original Title

Cdk13-/- Mice Exhibit Developmental Delay and Craniofacial Malformations during Embryonic Development

Type

presentation, poster

Language

English

Original Abstract

Cyclin-dependent kinase 13 (CDK13) belongs to the family of transcription regulating kinases. Together with its binding partners, cyclin K or L, they form a complex which regulates phosphorylation of RNA Polymerase II, or control alternative splicing. Large numbers of different mutations of this gene cause various developmental defects. In humans, these mutations cause developmental delay, intellectual disability, autism, seizures, facial dysmorphisms, structural heart, brain and digital abnormalities. Our mouse strain with mutation in Cdk13 gene has very similar phenotypic manifestations including developmental delay, craniofacial and heart abnormalities, plus defects in kidney morphology. The aim of this study is to precisely describe morphological changes in the craniofacial region of Cdk13-/- embryos and to reveal what cellular and molecular processes are responsible for these changes. According to macroscopic and microscopic analysis, the most obvious morphological differences between wild type and mutant embryos in the craniofacial region are a generally smaller head, cleft palate and smaller and dysmorphic incisor tooth germs. Alizarin red and Alcian blue staining showed differences in morphology of bones and cartilages of the head between wild type and mutant embryos. For deeper analysis of bones and teeth, we performed μCTscanning. Analyses were performed on embryos from E11.5 to E16.5. Precursor cells normally migrate along the axons to their final destination in order to differentiate and form a specific tissue or can serve there as a source for eventual renewal. Our goal is to reveal whether migration of craniofacial-forming cells is impeded if axonal outgrowth in Cdk13 mutants is defective. CDK13 is known to be responsible for axon outgrowth in vitro. This hypothesis will be verified using IHC on slides and on wholemount embryos, and on PCR arrays specific for mouse neurogenesis markers.

Keywords

Conference poster

Authors

HAMPL, M.; KAVKOVÁ, M.; ZIKMUND, T.; KAISER, J.; BUCHTOVÁ, M.

Released

3. 6. 2019

Publisher

Wiley

ISBN

0362-2525

Periodical

JOURNAL OF MORPHOLOGY

Year of study

280

State

United States of America

Pages from

131

Pages to

131

Pages count

244

BibTex

@misc{BUT157861,
  author="Marek {Hampl} and Michaela {Kavková} and Tomáš {Zikmund} and Jozef {Kaiser} and Marcela {Buchtová}",
  title="Cdk13-/- Mice Exhibit Developmental Delay and Craniofacial Malformations during Embryonic Development",
  year="2019",
  journal="JOURNAL OF MORPHOLOGY",
  volume="280",
  pages="131--131",
  publisher="Wiley",
  issn="0362-2525",
  note="presentation, poster"
}