Brief Report: Isogenic Induced Pluripotent Stem Cell Lines From an Adult With Mosaic Down Syndrome Model Accelerated Neuronal Ageing and Neurodegeneration

Author:

Murray Aoife12,Letourneau Audrey3,Canzonetta Claudia1,Stathaki Elisavet4,Gimelli Stefania4,Sloan-Bena Frederique4,Abrehart Robert1,Goh Pollyanna12,Lim Shuhui5,Baldo Chiara6,Dagna-Bricarelli Franca7,Hannan Saad8,Mortensen Martin8,Ballard David9,Syndercombe Court Denise9,Fusaki Noemi10,Hasegawa Mamoru11,Smart Trevor G.8,Bishop Cleo1,Antonarakis Stylianos E.3,Groet Jürgen1212,Nizetic Dean125

Affiliation:

1. The Blizard Institute Barts and The London School of Medicine, London, United Kingdom

2. The LonDownS Consortium, Wellcome Trust, London, United Kingdom

3. Department of Genetic Medicine and Development University of Geneva Medical School, Geneva, Switzerland

4. Service of Genetic Medicine, University Geneva Hospitals, Geneva, Switzerland

5. Lee Kong Chian School of Medicine, Nanyang Technological University, Singapore, Singapore

6. Human Genetics Laboratory, Galliera Hospital, Genoa, Italy

7. Liguria Department of Genetics, Genoa, Italy

8. Department of Neuroscience, Physiology and Pharmacology University College London, London, United Kingdom

9. Department of Forensic and Analytical Science King's College, London, United Kingdom

10. Precursory Research for Embryonic Science and Technology, Japan Science and Technology Agency, Saitama, Japan

11. DNAVEC Corporation, Ibaraki, Tokyo, Japan

12. Stem Cell Laboratory, National Centre for Bowel Research and Surgical Innovation, Queen Mary University of London, London, United Kingdom

Abstract

Abstract Trisomy 21 (T21), Down Syndrome (DS) is the most common genetic cause of dementia and intellectual disability. Modeling DS is beginning to yield pharmaceutical therapeutic interventions for amelioration of intellectual disability, which are currently being tested in clinical trials. DS is also a unique genetic system for investigation of pathological and protective mechanisms for accelerated ageing, neurodegeneration, dementia, cancer, and other important common diseases. New drugs could be identified and disease mechanisms better understood by establishment of well-controlled cell model systems. We have developed a first nonintegration-reprogrammed isogenic human induced pluripotent stem cell (iPSC) model of DS by reprogramming the skin fibroblasts from an adult individual with constitutional mosaicism for DS and separately cloning multiple isogenic T21 and euploid (D21) iPSC lines. Our model shows a very low number of reprogramming rearrangements as assessed by a high-resolution whole genome CGH-array hybridization, and it reproduces several cellular pathologies seen in primary human DS cells, as assessed by automated high-content microscopic analysis. Early differentiation shows an imbalance of the lineage-specific stem/progenitor cell compartments: T21 causes slower proliferation of neural and faster expansion of hematopoietic lineage. T21 iPSC-derived neurons show increased production of amyloid peptide-containing material, a decrease in mitochondrial membrane potential, and an increased number and abnormal appearance of mitochondria. Finally, T21-derived neurons show significantly higher number of DNA double-strand breaks than isogenic D21 controls. Our fully isogenic system therefore opens possibilities for modeling mechanisms of developmental, accelerated ageing, and neurodegenerative pathologies caused by T21. Stem Cells  2015;33:2077–2084 Video Highlight: https://youtu.be/MoMwXg2azGo

Funder

Wellcome Trust

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Developmental Biology,Molecular Medicine

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