Embryonic statistical analyses reveal 2 growth phenotypes in mouse models of Down syndrome - 24/01/24
, Lauren Bishop, MD c, f, Taisuke Sato, MD, PhD a, Laura L. Baxter, PhD a, Victoria Hoffmann, DVM d, Laura Koehly, PhD b, Faycal Guedj, PhD aAbstract |
Background |
Down syndrome is associated with several comorbidities, including intellectual disability, growth restriction, and congenital heart defects. The prevalence of Down syndrome–associated comorbidities is highly variable, and intellectual disability, although fully penetrant, ranges from mild to severe. Understanding the basis of this interindividual variability might identify predictive biomarkers of in utero and postnatal outcomes that could be used as endpoints to test the efficacy of future therapeutic interventions.
Objective |
The main objective of this study was to examine if antenatal interindividual variability exists in mouse models of Down syndrome and whether applying statistical approaches to clinically relevant measurements (ie, the weights of the embryo, placenta, and brain) could define cutoffs that discriminate between subgroups of trisomic embryos.
Study Design |
Three commonly used mouse models of Down syndrome (Dp(16)1/Yey, Ts65Dn, and Ts1Cje) and a new model (Ts66Yah) were used in this study. Trisomic and euploid littermate embryos were used from each model with total numbers of 102 for Ts66Yah, 118 for Dp(16)1/Yey, 92 for Ts65Dn, and 126 for Ts1Cje. Placental, embryonic, and brain weights and volumes at embryonic day 18.5 were compared between genotypes in each model. K-mean clustering analysis was applied to embryonic and brain weights to identify severity classes in trisomic embryos, and brain and placental volumetric measurements were compared between genotypes and classes for each strain. In addition, Ts66Yah embryos were examined for malformations because embryonic phenotypes have never been examined in this model.
Results |
Reduced body and brain weights were present in Ts66Yah, Dp(16)1/Yey, and Ts65Dn embyos. Cluster analysis identified 2 severity classes in trisomic embryos—mild and severe—in all 4 models that were distinguishable using a putative embryonic weight cutoff of <0.5 standard deviation below the mean. Ts66Yah trisomic embryos develop congenital anomalies that are also found in humans with Down syndrome, including congenital heart defects and renal pelvis dilation.
Conclusion |
Statistical approaches applied to clinically relevant measurements revealed 2 classes of phenotypic severity in trisomic mouse models of Down syndrome. Analysis of severely affected trisomic animals may facilitate the identification of biomarkers and endpoints that can be used to prenatally predict outcomes and the efficacy of treatments.
Le texte complet de cet article est disponible en PDF.Key words : biomarkers, Down syndrome, fetal growth, mouse models, phenotype severity, placental development, Ts66Yah
Plan
| A.D.A. and J.L. contributed equally to this study. |
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| The authors report no conflict of interest. |
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| This research study was supported by the Intramural Research Program of the National Human Genome Research Institute, National Institutes of Health under grant number ZIA HG200399-05. |
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| All data generated or analyzed during this study were included in this published article and its supplementary information files. |
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| This study was carried out in strict accordance with the recommendations stipulated in the Guide for the Care and Use of Laboratory Animals of the National Institutes of Health. All experimental procedures [NHGRI Protocol G-17-1] were approved by the Institutional Animal Care and Use Committee. |
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| Cite this article as: Adams AD, Lin J, Bianchi DW, et al. Embryonic statistical analyses reveal 2 growth phenotypes in mouse models of Down syndrome. Am J Obstet Gynecol 2024;230:258.e1-11. |
Vol 230 - N° 2
P. 258.e1-258.e11 - février 2024 Retour au numéro
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