2017
DOI: 10.1016/j.nbd.2016.12.009
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A codon-optimized Mecp2 transgene corrects breathing deficits and improves survival in a mouse model of Rett syndrome

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Cited by 39 publications
(42 citation statements)
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“…Importantly, however, intracisternal administration of 1 × 10 12 vg AAV9/ hMECP2 (v1) still resulted in potentially problematic peripheral transgene expression (Figure 2), a trend toward elevated blood serum toxicity indicators (Figure S2), and deleterious neurological side effects (Figures 1 and 3), which were not seen in mice treated with an AAV9/EGFP control vector. Increased severity of hindlimb clasping and abnormal gait were unexpected, given the absence of these side effects in previously published MeCP2 gene transfer studies 11, 12, 32. In light of these data, our conclusion is that AAV9/ hMECP2 (v1) cannot move forward in translational studies.…”
Section: Discussionmentioning
confidence: 60%
“…Importantly, however, intracisternal administration of 1 × 10 12 vg AAV9/ hMECP2 (v1) still resulted in potentially problematic peripheral transgene expression (Figure 2), a trend toward elevated blood serum toxicity indicators (Figure S2), and deleterious neurological side effects (Figures 1 and 3), which were not seen in mice treated with an AAV9/EGFP control vector. Increased severity of hindlimb clasping and abnormal gait were unexpected, given the absence of these side effects in previously published MeCP2 gene transfer studies 11, 12, 32. In light of these data, our conclusion is that AAV9/ hMECP2 (v1) cannot move forward in translational studies.…”
Section: Discussionmentioning
confidence: 60%
“…Recent attempts to deliver MECP2 exogenously in mouse models of RTT used widely varying vector doses but are difficult to compare based on additional differences in cassette design and other variables, including viral production, dosing protocol, and phenotype measures 19, 20, 21. In the present study, we used our previously published cassette design (human MECP2_e1 , under the control of a MeP229 core promoter fragment) 19 to directly investigate the effect of dose in terms of efficacy and safety.…”
Section: Discussionmentioning
confidence: 99%
“…Previous preclinical RTT gene therapy studies19, 20, 21 have focused on using the Mecp2 − /y model to screen for vector efficacy and potential toxicity. However, the presence of mutant endogenous MeCP2 could potentially produce a quasi-dominant negative action on the vector-derived MeCP2.…”
Section: Discussionmentioning
confidence: 99%
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“…Thus, a successful gene therapy for RTT has to deliver the correct MeCP2 dosage in a tight range that overlaps with endogenous levels. Different studies have recently provided encouraging results showing that intravenous administration of an Adeno-associated virus serotype 9 (AAV9) expressing the wild-type (WT) MECP2 attenuated neurological dysfunctions and extended lifespan in RTT mice [14][15][16][17] . However, the AAV9 does not cross efficiently the blood-brain barrier in adult mice while having a preferential tropism for peripheral organs.…”
Section: Introductionmentioning
confidence: 99%