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Research ArticleFailure to Replicate, Sensory and Motor Systems

Experimental Design and Data Analysis Issues Contribute to Inconsistent Results of C-Bouton Changes in Amyotrophic Lateral Sclerosis

S. Shekar Dukkipati, Aouatef Chihi, Yiwen Wang and Sherif M. Elbasiouny
eNeuro 6 January 2017, 4 (1) ENEURO.0281-16.2016; DOI: https://doi.org/10.1523/ENEURO.0281-16.2016
S. Shekar Dukkipati
1Department of Neuroscience, Cell Biology, and Physiology, Boonshoft School of Medicine and College of Science and Mathematics, Wright State University, Dayton, Ohio 45435
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Aouatef Chihi
2Department of Biomedical, Industrial, and Human Factors Engineering, College of Engineering and Computer Science, Wright State University, Dayton, Ohio 45435
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Yiwen Wang
2Department of Biomedical, Industrial, and Human Factors Engineering, College of Engineering and Computer Science, Wright State University, Dayton, Ohio 45435
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Sherif M. Elbasiouny
1Department of Neuroscience, Cell Biology, and Physiology, Boonshoft School of Medicine and College of Science and Mathematics, Wright State University, Dayton, Ohio 45435
2Department of Biomedical, Industrial, and Human Factors Engineering, College of Engineering and Computer Science, Wright State University, Dayton, Ohio 45435
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Abstract

The possible presence of pathological changes in cholinergic synaptic inputs [cholinergic boutons (C-boutons)] is a contentious topic within the ALS field. Conflicting data reported on this issue makes it difficult to assess the roles of these synaptic inputs in ALS. Our objective was to determine whether the reported changes are truly statistically and biologically significant and why replication is problematic. This is an urgent question, as C-boutons are an important regulator of spinal motoneuron excitability, and pathological changes in motoneuron excitability are present throughout disease progression. Using male mice of the SOD1-G93A high-expresser transgenic (G93A) mouse model of ALS, we examined C-boutons on spinal motoneurons. We performed histological analysis at high statistical power, which showed no difference in C-bouton size in G93A versus wild-type motoneurons throughout disease progression. In an attempt to examine the underlying reasons for our failure to replicate reported changes, we performed further histological analyses using several variations on experimental design and data analysis that were reported in the ALS literature. This analysis showed that factors related to experimental design, such as grouping unit, sampling strategy, and blinding status, potentially contribute to the discrepancy in published data on C-bouton size changes. Next, we systematically analyzed the impact of study design variability and potential bias on reported results from experimental and preclinical studies of ALS. Strikingly, we found that practices such as blinding and power analysis are not systematically reported in the ALS field. Protocols to standardize experimental design and minimize bias are thus critical to advancing the ALS field.

  • ALS
  • amyotrophic lateral sclerosis
  • C-bouton
  • cholinergic synapse
  • motoneuron
  • SOD1-G93A

Footnotes

  • The authors declare no competing financial interests.

  • This project was funded by National Institutes of Health Grant NS091836. A.C. was supported through the NIH/NIGMS R25GM090122, IMSD BioSTAR program grant at Wright State University.

This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International, which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.

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eneuro: 4 (1)
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January/February 2017
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Experimental Design and Data Analysis Issues Contribute to Inconsistent Results of C-Bouton Changes in Amyotrophic Lateral Sclerosis
S. Shekar Dukkipati, Aouatef Chihi, Yiwen Wang, Sherif M. Elbasiouny
eNeuro 6 January 2017, 4 (1) ENEURO.0281-16.2016; DOI: 10.1523/ENEURO.0281-16.2016

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Experimental Design and Data Analysis Issues Contribute to Inconsistent Results of C-Bouton Changes in Amyotrophic Lateral Sclerosis
S. Shekar Dukkipati, Aouatef Chihi, Yiwen Wang, Sherif M. Elbasiouny
eNeuro 6 January 2017, 4 (1) ENEURO.0281-16.2016; DOI: 10.1523/ENEURO.0281-16.2016
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Keywords

  • ALS
  • amyotrophic lateral sclerosis
  • C-bouton
  • cholinergic synapse
  • motoneuron
  • SOD1-G93A

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