Corrigendum to: Posttranscriptional regulation of colonic epithelial repair by RNA binding protein IMP 1/ IGF 2 BP 1 (EMBO reports, (2019), 20, 6, 10.15252/embr.201847074)

Priya Chatterji; Patrick A. Williams; Kelly A. Whelan; Fernando C. Samper; Sarah F. Andres; Lauren A. Simon; Louis R. Parham; Rei Mizuno; Emma T. Lundsmith; David S.M. Lee; Shun Liang; HR Sagara Wijeratne; Stefanie Marti; Lillian Chau; Veronique Giroux; Benjamin J. Wilkins; Gary D. Wu; Premal Shah; Gian G. Tartaglia; Kathryn E. Hamilton

doi:10.15252/embr.202153324

Corrigendum to: Posttranscriptional regulation of colonic epithelial repair by RNA binding protein IMP 1/ IGF 2 BP 1 (EMBO reports, (2019), 20, 6, 10.15252/embr.201847074)

Priya Chatterji, Patrick A. Williams, Kelly A. Whelan, Fernando C. Samper, Sarah F. Andres, Lauren A. Simon, Louis R. Parham, Rei Mizuno, Emma T. Lundsmith, David S.M. Lee, Shun Liang, HR Sagara Wijeratne, Stefanie Marti, Lillian Chau, Veronique Giroux, Benjamin J. Wilkins, Gary D. Wu, Premal Shah, Gian G. Tartaglia, Kathryn E. Hamilton

Research output: Contribution to journal › Comment/debate › peer-review

4 Scopus citations

Abstract

The authors noticed that the control and disease labels had been inverted in their data analysis resulting in publication of incorrect data in Figure 1C. The corrected figure is displayed below. This change affects the conclusions as detailed below. The authors apologize for this error and any confusion it may have caused. In the legend of 1C, change from, “Differential gene expression analysis of pediatric ileal CD patient samples (n = 180) shows increased (> 4-fold) IMP1 expression as compared to non-inflammatory bowel disease (IBD) pediatric samples (n = 43)”. To, "Differential gene expression analysis of pediatric ileal CD patient samples (n = 180) shows decreased (> 4-fold) IMP1 expression as compared to non-inflammatory bowel disease (IBD) pediatric samples (n = 43)”. In abstract, change from, “Here, we report increased IMP1 expression in patients with Crohn’s disease and ulcerative colitis”. To, “Here, we report increased IMP1 expression in adult patients with Crohn’s disease and ulcerative colitis”. In results, change from, “Consistent with these findings, analysis of published the Pediatric RISK Stratification Study (RISK) cohort of RNA-sequencing data 38 from pediatric patients with Crohn’s disease (CD) patients revealed that IMP1 is upregulated significantly compared to control patients and that this effect is specific to IMP1 (i.e., other distinct isoforms, IMP2 and IMP3, are not changed; Fig 1C)”. To, “Contrary to our findings in colon tissue from adults, analysis of published RNA-sequencing data from the Pediatric RISK Stratification Study (RISK) cohort of ileal tissue from children with Crohn’s disease (CD) 38 revealed that IMP1 is downregulated significantly compared to control patients in the RISK cohort and that this effect is specific to IMP1 (i.e., other distinct isoforms, IMP2 and IMP3, are not changed; Fig 1C)”. (Figure presented.) In discussion, change from, “Indeed, we report that IMP1 is upregulated in patients with Crohn’s disease and ulcerative colitis and that mice with Imp1 loss exhibit enhanced repair following DSSmediated damage”. To “Indeed, we report that IMP1 is upregulated in adult patients with Crohn’s disease and ulcerative colitis and that mice with Imp1 loss exhibit enhanced repair following DSS-mediated damage”.

Original language	English (US)
Article number	e47074
Journal	EMBO Reports
Volume	22
Issue number	8
DOIs	https://doi.org/10.15252/embr.202153324
State	Published - Aug 4 2021

ASJC Scopus subject areas

Biochemistry
Molecular Biology
Genetics

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10.15252/embr.202153324

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Chatterji, P., Williams, P. A., Whelan, K. A., Samper, F. C., Andres, S. F., Simon, L. A., Parham, L. R., Mizuno, R., Lundsmith, E. T., Lee, D. S. M., Liang, S., Wijeratne, HRS., Marti, S., Chau, L., Giroux, V., Wilkins, B. J., Wu, G. D., Shah, P., Tartaglia, G. G., & Hamilton, K. E. (2021). Corrigendum to: Posttranscriptional regulation of colonic epithelial repair by RNA binding protein IMP 1/ IGF 2 BP 1 (EMBO reports, (2019), 20, 6, 10.15252/embr.201847074). EMBO Reports, 22(8), Article e47074. https://doi.org/10.15252/embr.202153324

Chatterji, P, Williams, PA, Whelan, KA, Samper, FC, Andres, SF, Simon, LA, Parham, LR, Mizuno, R, Lundsmith, ET, Lee, DSM, Liang, S, Wijeratne, HRS, Marti, S, Chau, L, Giroux, V, Wilkins, BJ, Wu, GD, Shah, P, Tartaglia, GG & Hamilton, KE 2021, 'Corrigendum to: Posttranscriptional regulation of colonic epithelial repair by RNA binding protein IMP 1/ IGF 2 BP 1 (EMBO reports, (2019), 20, 6, 10.15252/embr.201847074)', EMBO Reports, vol. 22, no. 8, e47074. https://doi.org/10.15252/embr.202153324

@article{3643d97e72f14b6cb900df0c8f0262ea,

title = "Corrigendum to: Posttranscriptional regulation of colonic epithelial repair by RNA binding protein IMP 1/ IGF 2 BP 1 (EMBO reports, (2019), 20, 6, 10.15252/embr.201847074)",

abstract = "The authors noticed that the control and disease labels had been inverted in their data analysis resulting in publication of incorrect data in Figure 1C. The corrected figure is displayed below. This change affects the conclusions as detailed below. The authors apologize for this error and any confusion it may have caused. In the legend of 1C, change from, “Differential gene expression analysis of pediatric ileal CD patient samples (n = 180) shows increased (> 4-fold) IMP1 expression as compared to non-inflammatory bowel disease (IBD) pediatric samples (n = 43)”. To, {"}Differential gene expression analysis of pediatric ileal CD patient samples (n = 180) shows decreased (> 4-fold) IMP1 expression as compared to non-inflammatory bowel disease (IBD) pediatric samples (n = 43)”. In abstract, change from, “Here, we report increased IMP1 expression in patients with Crohn{\textquoteright}s disease and ulcerative colitis”. To, “Here, we report increased IMP1 expression in adult patients with Crohn{\textquoteright}s disease and ulcerative colitis”. In results, change from, “Consistent with these findings, analysis of published the Pediatric RISK Stratification Study (RISK) cohort of RNA-sequencing data 38 from pediatric patients with Crohn{\textquoteright}s disease (CD) patients revealed that IMP1 is upregulated significantly compared to control patients and that this effect is specific to IMP1 (i.e., other distinct isoforms, IMP2 and IMP3, are not changed; Fig 1C)”. To, “Contrary to our findings in colon tissue from adults, analysis of published RNA-sequencing data from the Pediatric RISK Stratification Study (RISK) cohort of ileal tissue from children with Crohn{\textquoteright}s disease (CD) 38 revealed that IMP1 is downregulated significantly compared to control patients in the RISK cohort and that this effect is specific to IMP1 (i.e., other distinct isoforms, IMP2 and IMP3, are not changed; Fig 1C)”. (Figure presented.) In discussion, change from, “Indeed, we report that IMP1 is upregulated in patients with Crohn{\textquoteright}s disease and ulcerative colitis and that mice with Imp1 loss exhibit enhanced repair following DSSmediated damage”. To “Indeed, we report that IMP1 is upregulated in adult patients with Crohn{\textquoteright}s disease and ulcerative colitis and that mice with Imp1 loss exhibit enhanced repair following DSS-mediated damage”.",

author = "Priya Chatterji and Williams, {Patrick A.} and Whelan, {Kelly A.} and Samper, {Fernando C.} and Andres, {Sarah F.} and Simon, {Lauren A.} and Parham, {Louis R.} and Rei Mizuno and Lundsmith, {Emma T.} and Lee, {David S.M.} and Shun Liang and HR Sagara Wijeratne and Stefanie Marti and Lillian Chau and Veronique Giroux and Wilkins, {Benjamin J.} and Wu, {Gary D.} and Premal Shah and Tartaglia, {Gian G.} and Hamilton, {Kathryn E.}",

note = "Publisher Copyright: {\textcopyright} 2021 The Authors.",

year = "2021",

month = aug,

day = "4",

doi = "10.15252/embr.202153324",

language = "English (US)",

volume = "22",

journal = "EMBO Reports",

issn = "1469-221X",

publisher = "Nature Publishing Group",

number = "8",

}

TY - JOUR

T1 - Corrigendum to

T2 - Posttranscriptional regulation of colonic epithelial repair by RNA binding protein IMP 1/ IGF 2 BP 1 (EMBO reports, (2019), 20, 6, 10.15252/embr.201847074)

AU - Chatterji, Priya

AU - Williams, Patrick A.

AU - Whelan, Kelly A.

AU - Samper, Fernando C.

AU - Andres, Sarah F.

AU - Simon, Lauren A.

AU - Parham, Louis R.

AU - Mizuno, Rei

AU - Lundsmith, Emma T.

AU - Lee, David S.M.

AU - Liang, Shun

AU - Wijeratne, HR Sagara

AU - Marti, Stefanie

AU - Chau, Lillian

AU - Giroux, Veronique

AU - Wilkins, Benjamin J.

AU - Wu, Gary D.

AU - Shah, Premal

AU - Tartaglia, Gian G.

AU - Hamilton, Kathryn E.

PY - 2021/8/4

Y1 - 2021/8/4

N2 - The authors noticed that the control and disease labels had been inverted in their data analysis resulting in publication of incorrect data in Figure 1C. The corrected figure is displayed below. This change affects the conclusions as detailed below. The authors apologize for this error and any confusion it may have caused. In the legend of 1C, change from, “Differential gene expression analysis of pediatric ileal CD patient samples (n = 180) shows increased (> 4-fold) IMP1 expression as compared to non-inflammatory bowel disease (IBD) pediatric samples (n = 43)”. To, "Differential gene expression analysis of pediatric ileal CD patient samples (n = 180) shows decreased (> 4-fold) IMP1 expression as compared to non-inflammatory bowel disease (IBD) pediatric samples (n = 43)”. In abstract, change from, “Here, we report increased IMP1 expression in patients with Crohn’s disease and ulcerative colitis”. To, “Here, we report increased IMP1 expression in adult patients with Crohn’s disease and ulcerative colitis”. In results, change from, “Consistent with these findings, analysis of published the Pediatric RISK Stratification Study (RISK) cohort of RNA-sequencing data 38 from pediatric patients with Crohn’s disease (CD) patients revealed that IMP1 is upregulated significantly compared to control patients and that this effect is specific to IMP1 (i.e., other distinct isoforms, IMP2 and IMP3, are not changed; Fig 1C)”. To, “Contrary to our findings in colon tissue from adults, analysis of published RNA-sequencing data from the Pediatric RISK Stratification Study (RISK) cohort of ileal tissue from children with Crohn’s disease (CD) 38 revealed that IMP1 is downregulated significantly compared to control patients in the RISK cohort and that this effect is specific to IMP1 (i.e., other distinct isoforms, IMP2 and IMP3, are not changed; Fig 1C)”. (Figure presented.) In discussion, change from, “Indeed, we report that IMP1 is upregulated in patients with Crohn’s disease and ulcerative colitis and that mice with Imp1 loss exhibit enhanced repair following DSSmediated damage”. To “Indeed, we report that IMP1 is upregulated in adult patients with Crohn’s disease and ulcerative colitis and that mice with Imp1 loss exhibit enhanced repair following DSS-mediated damage”.

AB - The authors noticed that the control and disease labels had been inverted in their data analysis resulting in publication of incorrect data in Figure 1C. The corrected figure is displayed below. This change affects the conclusions as detailed below. The authors apologize for this error and any confusion it may have caused. In the legend of 1C, change from, “Differential gene expression analysis of pediatric ileal CD patient samples (n = 180) shows increased (> 4-fold) IMP1 expression as compared to non-inflammatory bowel disease (IBD) pediatric samples (n = 43)”. To, "Differential gene expression analysis of pediatric ileal CD patient samples (n = 180) shows decreased (> 4-fold) IMP1 expression as compared to non-inflammatory bowel disease (IBD) pediatric samples (n = 43)”. In abstract, change from, “Here, we report increased IMP1 expression in patients with Crohn’s disease and ulcerative colitis”. To, “Here, we report increased IMP1 expression in adult patients with Crohn’s disease and ulcerative colitis”. In results, change from, “Consistent with these findings, analysis of published the Pediatric RISK Stratification Study (RISK) cohort of RNA-sequencing data 38 from pediatric patients with Crohn’s disease (CD) patients revealed that IMP1 is upregulated significantly compared to control patients and that this effect is specific to IMP1 (i.e., other distinct isoforms, IMP2 and IMP3, are not changed; Fig 1C)”. To, “Contrary to our findings in colon tissue from adults, analysis of published RNA-sequencing data from the Pediatric RISK Stratification Study (RISK) cohort of ileal tissue from children with Crohn’s disease (CD) 38 revealed that IMP1 is downregulated significantly compared to control patients in the RISK cohort and that this effect is specific to IMP1 (i.e., other distinct isoforms, IMP2 and IMP3, are not changed; Fig 1C)”. (Figure presented.) In discussion, change from, “Indeed, we report that IMP1 is upregulated in patients with Crohn’s disease and ulcerative colitis and that mice with Imp1 loss exhibit enhanced repair following DSSmediated damage”. To “Indeed, we report that IMP1 is upregulated in adult patients with Crohn’s disease and ulcerative colitis and that mice with Imp1 loss exhibit enhanced repair following DSS-mediated damage”.

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DO - 10.15252/embr.202153324

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SN - 1469-221X

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JO - EMBO Reports

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ER -

Corrigendum to: Posttranscriptional regulation of colonic epithelial repair by RNA binding protein IMP 1/ IGF 2 BP 1 (EMBO reports, (2019), 20, 6, 10.15252/embr.201847074)

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