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1. Comprehensive deletion landscape of CRISPR-Cas9 identifies minimal RNA-guided DNA-binding modules

2. Site-Specific Bioconjugation through Enzyme-Catalyzed Tyrosine–Cysteine Bond Formation

3. Loss of the neural-specific BAF subunit ACTL6B relieves repression of early response genes and causes recessive autism

4. CasX enzymes comprise a distinct family of RNA-guided genome editors.

5. A thermostable Cas9 with increased lifetime in human plasma.

6. Targeted gene knock-in by homology-directed genome editing using Cas9 ribonucleoprotein and AAV donor delivery

7. Efficient genome editing in the mouse brain by local delivery of engineered Cas9 ribonucleoprotein complexes

8. Profiling of engineering hotspots identifies an allosteric CRISPR-Cas9 switch

9. Rational design of a split-Cas9 enzyme complex

10. Enhanced homology-directed human genome engineering by controlled timing of CRISPR/Cas9 delivery.

15. MicroRNA-mediated switching of chromatin-remodelling complexes in neural development

22. Exome sequencing to identify de novo mutations in sporadic ALS trios

24. Kinetic Analysis of npBAF to nBAF Switching Reveals Exchange of SSI8 with CREST and Integration with Neural Developmental Pathways.

25. An embryonic stem cell chromatin remodeling complex, esBAF, is essential for embryonic stem cell self-renewal and pluripotency.

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