Literature DB >> 17428201

Effects of aneuploidy on skull growth in a mouse model of Down syndrome.

Cheryl A Hill1, Roger H Reeves, Joan T Richtsmeier.   

Abstract

Adult craniofacial morphology results from complex interactions among genetic, epigenetic and environmental factors. Trisomy causes perturbations in the genetic programmes that control development and these are reflected in morphology that can either ameliorate or worsen with time and growth. Many of the specific changes that occur in Down syndrome can be studied in the Ts65Dn trisomic mouse, which shows direct parallels with specific aspects of adult craniofacial dysmorphology associated with trisomy 21. This study investigates patterns of craniofacial growth in Ts65Dn mice and their euploid littermates to assess how the adult dysmorphology develops. Three-dimensional coordinate data were collected from microcomputed tomography scans of the face, cranial base, palate and mandible of newborn (P0) and adult trisomic and euploid mice. Growth patterns were analysed using Euclidean distance matrix analysis. P0 trisomic mice show significant differences in craniofacial shape. Growth is reduced along the rostro-caudal axis of the Ts65Dn face and palate relative to euploid littermates and Ts65Dn mandibles demonstrate reduced growth local to the mandibular processes. Thus, the features of Down syndrome that are reflected in the mature Ts65Dn skull are established early in development and growth does not appear to ameliorate them. Differences in growth may in fact contribute to many of the morphological differences that are evident at birth in trisomic mice and humans.

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Year:  2007        PMID: 17428201      PMCID: PMC2100298          DOI: 10.1111/j.1469-7580.2007.00705.x

Source DB:  PubMed          Journal:  J Anat        ISSN: 0021-8782            Impact factor:   2.610


  49 in total

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  25 in total

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Authors:  John M Starbuck; Tara Dutka; Tabetha S Ratliff; Roger H Reeves; Joan T Richtsmeier
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10.  Modulation of diabetes-induced palate defects by maternal immune stimulation.

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