Rescue of a Mouse Model of Spinal Muscular Atrophy With Respiratory Distress Type 1 by AAV9-IGHMBP2 Is Dose Dependent

Shababi, Monir; Feng, Zhichun; Villalón, Eric; Sibigtroth, Christine M; Osman, Erkan Y.; Miller, Madeline R.; Williams-Simon, Patricka A.; Lombardi, Abby; Sass, Thalia H; Atkinson, Arleigh K; Garcia, Michael L.; Ko, Chien‐Ping; Lorson, Christian L.

doi:10.1038/mt.2016.33

Cited by 29 publications

(49 citation statements)

References 34 publications

(49 reference statements)

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“…Gene therapy is the third possible approach to SMARD1 treatment, and its great advantage is that this therapy may have the potential to replace the deficient gene and restore a In two recent studies, Shababi and colleagues tested the ICV route (Shababi et al, 47 ) and compared this route with the IV route. 48 In the first paper, these authors treated mice by ICV injection with In conclusion, gene therapy seems to show encouraging results in laboratory and in vivo tests and thus requires great effort to reach the knowledge necessary to treat SMARD1.…”

Section: Gene Therapymentioning

confidence: 99%

“…In two recent studies, Shababi and colleagues tested the ICV route (Shababi et al, 47 ) and compared this route with the IV route. 48 In the first paper, these authors treated mice by ICV injection with 2 doses of virus (1.25 × 10 11 or 2.5 × 10 11 viral genomes, with the higher dose in a double volume of injection with a significant delay in the onset of dilated cardiomyopathy compared with that of the untreated controls.…”

Section: Gene Therapymentioning

confidence: 99%

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Spinal muscular atrophy with respiratory distress type 1: Clinical phenotypes, molecular pathogenesis and therapeutic insights

Saladini

Nizzardo

Govoni

et al. 2019

J Cellular Molecular Medi

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Spinal muscular atrophy with respiratory distress type 1 (SMARD1) is a rare autosomal recessive neuromuscular disorder caused by mutations in the IGHMBP2 gene, which encodes immunoglobulin μ-binding protein 2, leading to progressive spinal motor neuron degeneration. We review the data available in the literature about SMARD1. The vast majority of patients show an onset of typical symptoms in the first year of life. The main clinical features are distal muscular atrophy and diaphragmatic palsy, for which permanent supportive ventilation is required. No effective treatment is available yet, but novel therapeutic approaches, such as gene therapy, have shown encouraging results in preclinical settings and thus represent possible methods for treating SMARD1. Significant advancements in the understanding of both the SMARD1 clinical spectrum and its molecular mechanisms have allowed the rapid translation of preclinical therapeutic strategies to human patients to improve the poor prognosis of this devastating disease.

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Section: Gene Therapymentioning

confidence: 99%

Section: Gene Therapymentioning

confidence: 99%

Spinal muscular atrophy with respiratory distress type 1: Clinical phenotypes, molecular pathogenesis and therapeutic insights

Saladini

Nizzardo

Govoni

et al. 2019

J Cellular Molecular Medi

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“…Chociaż dokładny mechanizm prowadzący do degeneracji aksonów zarówno w SMARD1, jak i CMT nie jest poznany, wydaje się, że duże znaczenie odgrywa poziom białka IGHMBP2 w komórkach. W przypadku choroby CMT poziom białka oznaczanego metodą Western blot jest większy niż w SMARD1 [57,63].…”

Section: Choroba Charcot-marie-tooth Typu Aksonalnegounclassified

“…Prowadzone badania u chorych ze SMARD1, stanowią również szansę na skuteczną terapię w przypadku chorych z CMT2S. Jednak skuteczność tej terapii jest silnie zależna od dawki i przy wysokiej podaży wektora AAV9--IGHMBP2, może mieć skutki negatywne [63]. Zatem niezwykle ważne przy tej formie leczenia jest bardzo ścisłe dobranie dawki podawanego wektora, tak aby leczenie mogło być skutecznie lecz nietoksyczne.…”

Section: Próby Terapii Genowej W Cmtunclassified

Perspektywy terapii w polineuropatiach genetycznie uwarunkowanych

Kochański¹,

Kabzińska²,

Rzepnikowska³

et al. 2018

Postepy Biochem

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Polineuropatie genetycznie uwarunkowane (HMSN, ang. hereditary motor and sensory neuropathies) zwane również chorobami kręgu Charcot-Marie-Tooth (CMT) stanowią niezwykle heterogenną genetycznie (ponad 80 genów) grupę chorób obwodowego układu nerwowego człowieka. Istotą chorób kręgu CMT jest powolnie postępujący zanik mięśni dystalnych kończyn dolnych (podudzia) i górnych (przedramiona). Jak dotąd nie opracowano skutecznej metody leczenia CMT. W pracy przedstawiono obecny stan wiedzy dotyczący kliniki, patogenezy molekularnej i pierwszych prób terapeutycznych w CMT. Omówiono również możliwości wynikające z zastosowania modelu drożdżowego w poszukiwaniach nowych substancji leczniczych, jak i identyfikacji substancji neurotoksycznych.

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“… 14 , 16 The lifespan of nmd mice is variable, ranging from 10 weeks to 7 months. 14 , 17 , 18 A hallmark of the nmd phenotype includes hindlimb muscle weakness and retrenchment that appears within the second week of age and progresses to the forelimb and trunk muscles. 16 , 18 While cardiomyopathy is rarely reported in SMARD1 patients, it is a consistent phenotype observed in nmd mice.…”

Section: Introductionmentioning

confidence: 99%

A Direct Comparison of IV and ICV Delivery Methods for Gene Replacement Therapy in a Mouse Model of SMARD1

Shababi

Villalón

Kaifer

et al. 2018

Molecular Therapy - Methods & Clinical Development

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Spinal muscular atrophy with respiratory distress type 1 (SMARD1) is an infantile autosomal recessive disease caused by the loss of the ubiquitously expressed IGHMBP2 gene. SMARD1 causes degeneration of alpha-motor neurons, resulting in distal muscle weakness, diaphragm paralysis, and respiratory malfunction. We have reported that delivery of a low dose of AAV9-IGHMBP2 to the CNS results in a significant rescue of the SMARD1 mouse model (nmd). To examine how a delivery route can impact efficacy, a direct comparison of intravenous (IV) and intracerebroventricular (ICV) delivery of AAV9-IGHMBP2 was performed. Using a low-dose, both IV and ICV delivery routes led to a significant extension in survival and increased body weight. Conversely, only ICV-treated animals demonstrated improvements in the hindlimb muscle, neuromuscular junction, and motor function. The hindlimb phenotype of IV-treated mice resembled the untreated nmd mice. We investigated whether the increased survival of IV-treated nmd mice was the result of a positive impact on the cardiac function. Our results revealed that cardiac function and pathology were similarly improved in IV- and ICV-treated mice. We concluded that while IV delivery of a low dose does not improve the hindlimb phenotype and motor function, partial restoration of cardiac performance is sufficient to significantly extend survival.

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Rescue of a Mouse Model of Spinal Muscular Atrophy With Respiratory Distress Type 1 by AAV9-IGHMBP2 Is Dose Dependent

Cited by 29 publications

References 34 publications

Spinal muscular atrophy with respiratory distress type 1: Clinical phenotypes, molecular pathogenesis and therapeutic insights

Spinal muscular atrophy with respiratory distress type 1: Clinical phenotypes, molecular pathogenesis and therapeutic insights

Perspektywy terapii w polineuropatiach genetycznie uwarunkowanych

A Direct Comparison of IV and ICV Delivery Methods for Gene Replacement Therapy in a Mouse Model of SMARD1

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