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1. Recent Therapeutic Gene Editing Applications to Genetic Disorders

2. An Inducible Luminescent System to Explore Parkinson’s Disease-Associated Genes

3. Homozygous ALS-linked mutations in TARDBP/TDP-43 lead to hypoactivity and synaptic abnormalities in human iPSC-derived motor neurons

4. Disruption of DDX53 coding sequence has limited impact on iPSC-derived human NGN2 neurons

5. Transcriptional Dysregulation and Impaired Neuronal Activity in FMR1 Knock-Out and Fragile X Patients’ iPSC-Derived Models

6. Generation of patient-derived pluripotent stem cell-lines and CRISPR modified isogenic controls with mutations in the Parkinson’s associated GBA gene

7. Complete Disruption of Autism-Susceptibility Genes by Gene Editing Predominantly Reduces Functional Connectivity of Isogenic Human Neurons

8. Mutations in RAB39B in individuals with intellectual disability, autism spectrum disorder, and macrocephaly

9. CNTN5-/+or EHMT2-/+human iPSC-derived neurons from individuals with autism develop hyperactive neuronal networks

10. Homozygous ALS-linked mutations in TARDBP/TDP-43 lead to progressive synaptic dysfunction in human iPSC-derived motor neurons

11. Neuron-specific protein network mapping of autism risk genes identifies shared biological mechanisms and disease-relevant pathologies

12. Midbrain organoids with an SNCA gene triplication model key features of synucleinopathy

13. A streamlined CRISPR workflow to introduce mutations and generate isogenic iPSCs for modeling amyotrophic lateral sclerosis

14. Midbrain organoids with an

15. SHANK2 mutations associated with autism spectrum disorder cause hyperconnectivity of human neurons

16. Midbrain organoids with an SNCA gene triplication model key features of synucleinopathy

17. RNA-Seq reveals spliceosome and proteasome genes as most consistent transcripts in human cancer cells.

18. Complete Disruption of Autism-Susceptibility Genes by Gene Editing Predominantly Reduces Functional Connectivity of Isogenic Human Neurons

19. Synaptic dysfunction in human neurons with autism-associated deletions in PTCHD1-AS

20. CNTN5-/+or EHMT2-/+human iPSC-derived neurons from individuals with autism develop hyperactive neuronal networks

21. Author response: CNTN5-/+or EHMT2-/+human iPSC-derived neurons from individuals with autism develop hyperactive neuronal networks

22. CNTN5−/+orEHMT2−/+iPSC-Derived Neurons from Individuals with Autism Develop Hyperactive Neuronal Networks

23. Complete Disruption of Autism-Susceptibility Genes by Gene-Editing Predominantly Reduces Functional Connectivity of Isogenic Human Neurons

24. Mutations in RAB39B in individuals with intellectual disability, autism spectrum disorder, and macrocephaly

25. Whole-genome sequencing of quartet families with autism spectrum disorder

26. Whole genome sequencing resource identifies 18 new candidate genes for autism spectrum disorder

27. A role for GPx3 in activity of normal and leukemia stem cells

28. GPR56 identifies primary human acute myeloid leukemia cells with high repopulating potential in vivo

30. A Functional Screen to Identify Novel Effectors of Hematopoietic Stem Cell Activity

31. RNAi screen identifies Jarid1b as a major regulator of mouse HSC activity

32. RNA-Seq reveals spliceosome and proteasome genes as most consistent transcripts in human cancer cells

33. Genome-wide characteristics of de novo mutations in autism

34. Perturbation Of Gpsm2/Lgn Enhances Haematopoietic Stem Cell Function

35. Identification of non–cell-autonomous networks from engineered feeder cells that enhance murine hematopoietic stem cell activity

36. A Novel Osteoclastic Network Determines In Vitro Niche for Mouse and Human Hematopoietic Stem Cells

37. A Functional In Vivo RNAi screen Involving Jumonji C Domain Containing Candidates Unravels Kdm5b As a Negative Modulator of Hematopoietic Stem Cell Self-Renewal

38. Gpx3 Determines Competitiveness of Normal and Leukemic Stem Cells

39. A Functional Screen to Identify Novel Effectors of Hematopoietic Stem Cell Activity

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