A Pilot Study of the Effect of Gentamicin on Nasal  Potential Difference Measurements in Cystic Fibrosis  Patients Carrying Stop Mutations

Wilschanski, Michael; Famini, Chagit; Blau, Hannah; Rivlin, Joseph; Augarten, A.; Avital, Avraham; Kerem, Batsheva; Kerem, Eitan

doi:10.1164/ajrccm.161.3.9904116

Cited by 183 publications

(118 citation statements)

References 33 publications

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“…In our study, we focused on nonsense or frameshift mutations leading to PTC resulting in an almost complete absence of particular key proteins involved in lysosomal function and cell homeostasis maintenance. Preclinical studies with gentamicin or PTC124 had succeeded by enhancing stop codon readthrough and were able to be used as therapeutic agents for genetic diseases [9][10][11][12][13][14][15][16][17][18][36][37][38][39][40][41][42]. PTC124 has been successfully extended into clinical trials [18,43], although preliminary results are not clear for Duchenne muscular dystrophy [44].…”

Section: Discussionmentioning

confidence: 99%

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Effect of Readthrough Treatment in Fibroblasts of Patients Affected by Lysosomal Diseases Caused by Premature Termination Codons

et al. 2015

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Aminoglycoside antibiotics, such as gentamicin, may induce premature termination codon (PTC) readthrough and elude the nonsense-mediated mRNA decay mechanism. Because PTCs are frequently involved in lysosomal diseases, readthrough compounds may be useful as potential therapeutic agents. The aim of our study was to identify patients responsive to gentamicin treatment in order to be used as positive controls to further screen for other PTC readthrough compounds. With this aim, fibroblasts from 11 patients affected by 6 different lysosomal diseases carrying PTCs were treated with gentamicin. Treatment response was evaluated by measuring enzymatic activity, abnormal metabolite accumulation, mRNA expression, protein localization, and cell viability. The potential effect of readthrough was also analyzed by in silico predictions. Results showed that fibroblasts from 5/11 patients exhibited an up to 3-fold increase of enzymatic activity after gentamicin treatment. Accordingly, cell lines tested showed enhanced well-localized protein and/or increased mRNA expression levels and/or reduced metabolite accumulation. Interestingly, these cell lines also showed increased enzymatic activity after PTC124 treatment, which is a PTC readthroughpromoting compound. In conclusion, our results provide a proof-of-concept that PTCs can be effectively suppressed by readthrough drugs, with different efficiencies depending on the genetic context. The screening of new compounds with readthrough activity is a strategy that can be used to develop efficient therapies for diseases caused by PTC mutations.

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Section: Discussionmentioning

confidence: 99%

“…Glutamine is preferably inserted at nonsense UAG or UAA codons, whereas UGA miscode to tryptophan [36][37][38]. Taking into account these rules, the predicted amino acid changes were analyzed, using an in silico approach, for each patient (Polyphen-2 and SIFT analyses).…”

Section: In Silico Analysis Of the Predicted Substitutions Induced Bymentioning

confidence: 99%

Effect of Readthrough Treatment in Fibroblasts of Patients Affected by Lysosomal Diseases Caused by Premature Termination Codons

et al. 2015

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“…These results thus strongly suggest that only a subset of DMD and CMD patients carrying stop mutations would potentially benefit of a gentamicin treatment aiming at suppressing premature termination codons. They may also explain the failure or relative difficulty to obtain significant improvement of symptoms in clinical trials already reported, [34][35][36] since the patients included in these trials were not chosen on the criteria of the response of their mutation. Similarly, Gentamicin and muscular dystrophies L Bidou et al our efforts to correct the albino phenotype associated with the platinum (Typ cÀp ) coat color mutation by local or systemic treatment with gentamicin at several stages during embryogenesis, in pups and in adults failed (data not shown).…”

Section: Different Rules Govern Basal and Induced Readthroughmentioning

confidence: 99%

Premature stop codons involved in muscular dystrophies show a broad spectrum of readthrough efficiencies in response to gentamicin treatment

et al. 2004

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The suppression levels induced by gentamicin on premature stop codons, caused by primary nonsense mutations found in muscular dystrophy patients, were assessed using a very sensitive dual reporter gene assay. Results show that: (i) the effect of gentamicin on readthrough is similar in cultured cells and in vivo in murine skeletal muscle; (ii) a wide variability of readthrough efficiency is obtained, depending on the mutation tested; (iii) due to the complexity of readthrough regulation, efficiency cannot be predicted by the nucleotide context of the stop codon; (iv) only a minority of premature stop codons found in patients show a significant level of readthrough, and would thus be amenable to this pharmacological treatment, given our present understanding of the problem. These results probably provide an explanation for the relative failure of clinical trials reported to date using gentamicin to treat diseases due to premature stop codons, and emphasize that preliminary assays in cell culture provide valuable information concerning the potential efficiency of pharmacological treatments.

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“…However, other studies have reported neither the presence nor absence of gentamicin in the nucleus (Hashino et al 1997;Sundin et al 1997;Girton et al 2002). Nonetheless, a subset of cystic fibrosis patients can be partially rehabilitated through gentamicin therapy, which causes bypassing of the premature stop codon in the cystic fibrosis (CF) mutation, allowing functional transcription of the CF transmembrane protein (Howard et al 1996;Bedwell et al 1997;Wilschanski et al 2000;Clancy et al 2001;Du et al 2002;Zsembery et al 2002). This suggests that gentamicin can enter the nucleus.…”

Section: Consequences Of Gentamicin Accumulationmentioning

confidence: 99%

Uptake of Gentamicin by Bullfrog Saccular Hair Cells in vitro

Steyger

Peters

Rehling

et al. 2003

JARO - Journal of the Association for Research in Otolaryngolog

104

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Vertebrate sensory hair cells in the inner ear are pharmacologically sensitive to aminoglycoside antibiotics. Although the ototoxicity of aminoglycosides is well known, the route of drug uptake by hair cells and mechanisms of cytotoxicity remain poorly understood. Previously published studies have documented the intracellular distribution of gentamicin using immunocytochemical, electron microscopic, and autoradiographic methods. In this article, we compare the subcellular distribution of fluorescently conjugated gentamicin (gentamicin-Texas Red, GTTR) with immunolabeled gentamicin using confocal or electron microscopy. Gentamicin (detected by postfixation immunocytochemistry) and GTTR were rapidly taken up by hair cells throughout the bullfrog saccular explant in vitro and preferentially in peripheral hair cells. Immunolabeled gentamicin and GTTR were observed at the apical membranes of hair cells, particularly in their hair bundles. GTTR was also identified within a variety of subcellular compartments within hair cells, including lysosomes, mitochondria, Golgi bodies, endoplasmic reticulum, and nuclei, and in similar structures by immunoelectron microscopy. The distributions of GTTR and immunolabeled gentamicin are largely identical and corroborate a variety of published immunocytochemical and autoradiography studies. Thus, GTTR is a valid fluorescent probe with which to investigate the pharmacokinetics and mechanisms of gentamicin accumulation.

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A Pilot Study of the Effect of Gentamicin on Nasal Potential Difference Measurements in Cystic Fibrosis Patients Carrying Stop Mutations

Cited by 183 publications

References 33 publications

Effect of Readthrough Treatment in Fibroblasts of Patients Affected by Lysosomal Diseases Caused by Premature Termination Codons

Effect of Readthrough Treatment in Fibroblasts of Patients Affected by Lysosomal Diseases Caused by Premature Termination Codons

Premature stop codons involved in muscular dystrophies show a broad spectrum of readthrough efficiencies in response to gentamicin treatment

Uptake of Gentamicin by Bullfrog Saccular Hair Cells in vitro

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