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1. Antisense Oligonucleotide-mediated Suppression of Muscle Glycogen Synthase 1 Synthesis as an Approach for Substrate Reduction Therapy of Pompe Disease.

2. Systemic administration of AAV8-α-galactosidase A induces humoral tolerance in nonhuman primates despite low hepatic expression.

3. Induction of immune tolerance to a therapeutic protein by intrathymic gene delivery.

4. Preexisting immunity and low expression in primates highlight translational challenges for liver-directed AAV8-mediated gene therapy.

5. Evaluation of systemic follistatin as an adjuvant to stimulate muscle repair and improve motor function in Pompe mice.

6. Systemic Insulin-like growth factor-1 reverses hypoalgesia and improves mobility in a mouse model of diabetic peripheral neuropathy.

7. Timing of therapeutic intervention determines functional and survival outcomes in a mouse model of late infantile batten disease.

8. Local delivery of a viral vector mitigates neutralization by antiviral antibodies and results in efficient transduction of rabbit liver.

9. Transient siRNA-mediated attenuation of liver expression from an alpha-galactosidase A plasmid reduces subsequent humoral immune responses to the transgene product in mice.

10. Long-term transgene expression from plasmid DNA gene therapy vectors is negatively affected by CpG dinucleotides.

11. Contribution of Toll-like receptor 9 signaling to the acute inflammatory response to nonviral vectors.

12. Tumor treatment with complexes of cationic lipid and noncoding plasmid DNA results in the induction of cytotoxic T cells and systemic tumor elimination.

13. CpG-depleted plasmid DNA vectors with enhanced safety and long-term gene expression in vivo.

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