4.7 Article

Brachygnathia Inferior in Cloned Dogs Is Possibly Correlated with Variants of Wnt Signaling Pathway Initiators

Journal

Publisher

MDPI
DOI: 10.3390/ijms23010475

Keywords

cloned dog; brachygnathia inferior; whole-genome sequencing; Wnt signaling pathway

Funding

  1. Cooperative Research Program for Agriculture Science and Technology Development [PJ01092801]
  2. RDA, Republic of Korea

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Abnormalities have been reported in animals cloned via somatic cell nuclear transfer (SCNT). This study successfully cloned four healthy dogs for bomb-sniffing purposes, with two showing normal phenotypes and two showing abnormal mandible shortening. Genetic analysis revealed variants in Wnt signaling pathway initiators and cadherin in the cloned dogs with mandible shortening abnormalities.
Abnormalities in animals cloned via somatic cell nuclear transfer (SCNT) have been reported. In this study, to produce bomb-sniffing dogs, we successfully cloned four healthy dogs through SCNT using the same donor genome from the skin of a male German shepherd old dog. Veterinary diagnosis (X-ray/3D-CT imaging) revealed that two cloned dogs showed normal phenotypes, whereas the others showed abnormal shortening of the mandible (brachygnathia inferior) at 1 month after birth, even though they were cloned under the same conditions except for the oocyte source. Therefore, we aimed to determine the genetic cause of brachygnathia inferior in these cloned dogs. To determine the genetic defects related to brachygnathia inferior, we performed karyotyping and whole-genome sequencing (WGS) for identifying small genetic alterations in the genome, such as single-nucleotide variations or frameshifts. There were no chromosomal numerical abnormalities in all cloned dogs. However, WGS analysis revealed variants of Wnt signaling pathway initiators (WNT5B, DVL2, DACT1, ARRB2, FZD 4/8) and cadherin (CDH11, CDH1like) in cloned dogs with brachygnathia inferior. In conclusion, this study proposes that brachygnathia inferior in cloned dogs may be associated with variants in initiators and/or regulators of the Wnt/cadherin signaling pathway.

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