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A canine model of Cohen syndrome: Trapped Neutrophil Syndrome

Author: A Velayos-Baeza
AAG Aprikyan
Alan N Wilton
BA Neilan
BM vonHoldt
EA Ostrander
FJ Allan
HC Hennies
HG Parker
HG Parker
J Kolehmainen
J Kolehmainen
Jeremy R Shearman
JF Pang
JR Shearman
JR Shearman
KE Chandler
M Bugiani
M Silberstein
M Taban
MM Cohen Jr
S Kivitie-Kallio
S Kivitie-Kallio
S Rozen
SA Miller
W Seifert
W Seifert
WE Holmes
WS Oetting
Publication venue: BioMed Central
Publication date: 01/05/2011
Field of study

Abstract Background Trapped Neutrophil Syndrome (TNS) is a common autosomal recessive neutropenia in Border collie dogs. Results We used a candidate gene approach and linkage analysis to show that the causative gene for TNS is <it>VPS13B</it>. We chose <it>VPS13B </it>as a candidate because of similarities in clinical signs between TNS and Cohen syndrome, in human, such as neutropenia and a typical facial dysmorphism. Linkage analysis using microsatellites close to <it>VPS13B </it>showed positive linkage of the region to TNS. We sequenced each of the 63 exons of <it>VPS13B </it>in affected and control dogs and found that the causative mutation in Border collies is a 4 bp deletion in exon 19 of the largest transcript that results in premature truncation of the protein. Cohen syndrome patients present with mental retardation in 99% of cases, but learning disabilities featured in less than half of TNS affected dogs. It has been implied that loss of the alternate transcript of <it>VPS13B </it>in the human brain utilising an alternate exon, 28, may cause mental retardation. Mice cannot be used to test this hypothesis as they do not express the alternate exon. We show that dogs do express alternate transcripts in the brain utilising an alternate exon homologous to human exon 28. Conclusion Dogs can be used as a model organism to explore the function of the alternately spliced transcript of VPS13B in the brain. TNS in Border collies is the first animal model for Cohen syndrome and can be used to study the disease aetiology.</p

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PubMed Central

Periodontal status in two siblings with severe congenital neutropenia: Diagnosis and mutational analysis of the cases

Author: Aprikyan AAG
Ataoglu T
Aydinbelge M
Gokalp A
Guran S
hakkı sema
Koseoglu V
Somerman MJ
Ucar C
Yildirim S
Publication venue: 'American Academy of Periodontology (AAP)'
Publication date: 01/05/2005
Field of study

Background: Severe congenital neutropenia (SCN), also known as Kostmann syndrome, was originally reported as an autosomal recessive disease of neutrophil production. The disease is characterized by a maturation arrest of neutrophil precursors at the promyelocytic stage of differentiation and by extremely low levels of mature neutrophils in peripheral blood

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