The influence of genetic variation on late toxicities in childhood cancer survivors: A review

E. Clemens; A. L. F. van der Kooi; L. Broer; E. van Dulmen-den Broeder; H. Visscher; L. Kremer; W. Tissing; J. Loonen; C. M. Ronckers; S. M. F. Pluijm; S. J. C. M. M. Neggers; O. Zolk; T. Langer; A. am Zehnhoff-Dinnesen; C. L. Wilson; M. M. Hudson; B. Carleton; J. S. E. Laven; A. G. Uitterlinden; M. M. van den Heuvel-Eibrink

doi:10.1016/j.critrevonc.2018.04.001

The influence of genetic variation on late toxicities in childhood cancer survivors: A review

E. Clemens
, A. L. F. van der Kooi
, L. Broer
, E. van Dulmen-den Broeder
, H. Visscher
, L. Kremer
, W. Tissing
, J. Loonen
, C. M. Ronckers
, S. M. F. Pluijm
, S. J. C. M. M. Neggers
, O. Zolk
, T. Langer
, A. am Zehnhoff-Dinnesen
, C. L. Wilson
, M. M. Hudson
, B. Carleton
, J. S. E. Laven
, A. G. Uitterlinden
, M. M. van den Heuvel-Eibrink

Department of Pediatric Hematology and Oncology, Rotterdam, Netherlands
Princess Maxima Center for Pediatric Oncology, Utrecht, Netherlands
Department of Gynecology, Rotterdam, Netherlands
Department of Internal Medicine, Rotterdam, Netherlands
Radboud University Nijmegen Medical Centre
Transplant Surgery
Academic Medical Centre, University of Amsterdam
University of Groningen, University Medical Center Groningen
Maasstad Ziekenhuis
University Hospital of Ulm
Universitätsklinikum Schleswig-Holstein Campus Lübeck
University of Münster
St. Jude Children Research Hospital
University of British Columbia

Research output: Contribution to journal › Review article › Academic › peer-review

Abstract

Introduction: The variability in late toxicities among childhood cancer survivors (CCS) is only partially explained by treatment and baseline patient characteristics. Inter-individual variability in the association between treatment exposure and risk of late toxicity suggests that genetic variation possibly modifies this association. We reviewed the available literature on genetic susceptibility of late toxicity after childhood cancer treatment related to components of metabolic syndrome, bone mineral density, gonadal impairment and hearing impairment. Methods: A systematic literature search was performed, using Embase, Cochrane Library, Google Scholar, MEDLINE, and Web of Science databases. Eligible publications included all English language reports of candidate gene studies and genome wide association studies (GWAS) that aimed to identify genetic risk factors associated with the four late toxicities, defined as toxicity present after end of treatment. Results: Twenty-seven articles were identified, including 26 candidate gene studies: metabolic syndrome (n = 6); BMD (n = 6); gonadal impairment (n = 2); hearing impairment (n = 12) and one GWAS (metabolic syndrome). Eighty percent of the genetic studies on late toxicity after childhood cancer had relatively small sample sizes (n < 200), leading to insufficient power, and lacked adjustment for multiple comparisons. Only four (4/26 = 15%) candidate gene studies had their findings validated in independent replication cohorts as part of their own report. Conclusion: Genetic susceptibility associations are not consistent or not replicated and therefore, currently no evidence-based recommendations can be made for hearing impairment, gonadal impairment, bone mineral density impairment and metabolic syndrome in CCS. To advance knowledge related to genetic variation influencing late toxicities among CCS, future studies need adequate power, independent cohorts for replication, harmonization of disease outcomes and sample collections, and (international) collaboration.

Original language	English
Pages (from-to)	154-167
Journal	Critical reviews in oncology/hematology
Volume	126
DOIs	https://doi.org/10.1016/j.critrevonc.2018.04.001
Publication status	Published - 2018

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SDG 3 Good Health and Well-being

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10.1016/j.critrevonc.2018.04.001

Cite this

Clemens, E., van der Kooi, A. L. F., Broer, L., van Dulmen-den Broeder, E., Visscher, H., Kremer, L., Tissing, W., Loonen, J., Ronckers, C. M., Pluijm, S. M. F., Neggers, S. J. C. M. M., Zolk, O., Langer, T., Zehnhoff-Dinnesen, A. A., Wilson, C. L., Hudson, M. M., Carleton, B., Laven, J. S. E., Uitterlinden, A. G., & van den Heuvel-Eibrink, M. M. (2018). The influence of genetic variation on late toxicities in childhood cancer survivors: A review. Critical reviews in oncology/hematology, 126, 154-167. https://doi.org/10.1016/j.critrevonc.2018.04.001

@article{5e64b4575178401f931ca5dbf4e6bf00,

title = "The influence of genetic variation on late toxicities in childhood cancer survivors: A review",

abstract = "Introduction: The variability in late toxicities among childhood cancer survivors (CCS) is only partially explained by treatment and baseline patient characteristics. Inter-individual variability in the association between treatment exposure and risk of late toxicity suggests that genetic variation possibly modifies this association. We reviewed the available literature on genetic susceptibility of late toxicity after childhood cancer treatment related to components of metabolic syndrome, bone mineral density, gonadal impairment and hearing impairment. Methods: A systematic literature search was performed, using Embase, Cochrane Library, Google Scholar, MEDLINE, and Web of Science databases. Eligible publications included all English language reports of candidate gene studies and genome wide association studies (GWAS) that aimed to identify genetic risk factors associated with the four late toxicities, defined as toxicity present after end of treatment. Results: Twenty-seven articles were identified, including 26 candidate gene studies: metabolic syndrome (n = 6); BMD (n = 6); gonadal impairment (n = 2); hearing impairment (n = 12) and one GWAS (metabolic syndrome). Eighty percent of the genetic studies on late toxicity after childhood cancer had relatively small sample sizes (n < 200), leading to insufficient power, and lacked adjustment for multiple comparisons. Only four (4/26 = 15\%) candidate gene studies had their findings validated in independent replication cohorts as part of their own report. Conclusion: Genetic susceptibility associations are not consistent or not replicated and therefore, currently no evidence-based recommendations can be made for hearing impairment, gonadal impairment, bone mineral density impairment and metabolic syndrome in CCS. To advance knowledge related to genetic variation influencing late toxicities among CCS, future studies need adequate power, independent cohorts for replication, harmonization of disease outcomes and sample collections, and (international) collaboration.",

author = "E. Clemens and \{van der Kooi\}, \{A. L. F.\} and L. Broer and \{van Dulmen-den Broeder\}, E. and H. Visscher and L. Kremer and W. Tissing and J. Loonen and Ronckers, \{C. M.\} and Pluijm, \{S. M. F.\} and Neggers, \{S. J. C. M. M.\} and O. Zolk and T. Langer and Zehnhoff-Dinnesen, \{A. am\} and Wilson, \{C. L.\} and Hudson, \{M. M.\} and B. Carleton and Laven, \{J. S. E.\} and Uitterlinden, \{A. G.\} and \{van den Heuvel-Eibrink\}, \{M. M.\}",

year = "2018",

doi = "10.1016/j.critrevonc.2018.04.001",

language = "English",

volume = "126",

pages = "154--167",

journal = "Critical reviews in oncology/hematology",

issn = "1040-8428",

publisher = "Elsevier Ireland Ltd",

}

Clemens, E, van der Kooi, ALF, Broer, L, van Dulmen-den Broeder, E, Visscher, H, Kremer, L, Tissing, W, Loonen, J, Ronckers, CM, Pluijm, SMF, Neggers, SJCMM, Zolk, O, Langer, T, Zehnhoff-Dinnesen, AA, Wilson, CL, Hudson, MM, Carleton, B, Laven, JSE, Uitterlinden, AG & van den Heuvel-Eibrink, MM 2018, 'The influence of genetic variation on late toxicities in childhood cancer survivors: A review', Critical reviews in oncology/hematology, vol. 126, pp. 154-167. https://doi.org/10.1016/j.critrevonc.2018.04.001

TY - JOUR

T1 - The influence of genetic variation on late toxicities in childhood cancer survivors: A review

AU - Clemens, E.

AU - van der Kooi, A. L. F.

AU - Broer, L.

AU - van Dulmen-den Broeder, E.

AU - Visscher, H.

AU - Kremer, L.

AU - Tissing, W.

AU - Loonen, J.

AU - Ronckers, C. M.

AU - Pluijm, S. M. F.

AU - Neggers, S. J. C. M. M.

AU - Zolk, O.

AU - Langer, T.

AU - Zehnhoff-Dinnesen, A. am

AU - Wilson, C. L.

AU - Hudson, M. M.

AU - Carleton, B.

AU - Laven, J. S. E.

AU - Uitterlinden, A. G.

AU - van den Heuvel-Eibrink, M. M.

PY - 2018

Y1 - 2018

N2 - Introduction: The variability in late toxicities among childhood cancer survivors (CCS) is only partially explained by treatment and baseline patient characteristics. Inter-individual variability in the association between treatment exposure and risk of late toxicity suggests that genetic variation possibly modifies this association. We reviewed the available literature on genetic susceptibility of late toxicity after childhood cancer treatment related to components of metabolic syndrome, bone mineral density, gonadal impairment and hearing impairment. Methods: A systematic literature search was performed, using Embase, Cochrane Library, Google Scholar, MEDLINE, and Web of Science databases. Eligible publications included all English language reports of candidate gene studies and genome wide association studies (GWAS) that aimed to identify genetic risk factors associated with the four late toxicities, defined as toxicity present after end of treatment. Results: Twenty-seven articles were identified, including 26 candidate gene studies: metabolic syndrome (n = 6); BMD (n = 6); gonadal impairment (n = 2); hearing impairment (n = 12) and one GWAS (metabolic syndrome). Eighty percent of the genetic studies on late toxicity after childhood cancer had relatively small sample sizes (n < 200), leading to insufficient power, and lacked adjustment for multiple comparisons. Only four (4/26 = 15%) candidate gene studies had their findings validated in independent replication cohorts as part of their own report. Conclusion: Genetic susceptibility associations are not consistent or not replicated and therefore, currently no evidence-based recommendations can be made for hearing impairment, gonadal impairment, bone mineral density impairment and metabolic syndrome in CCS. To advance knowledge related to genetic variation influencing late toxicities among CCS, future studies need adequate power, independent cohorts for replication, harmonization of disease outcomes and sample collections, and (international) collaboration.

AB - Introduction: The variability in late toxicities among childhood cancer survivors (CCS) is only partially explained by treatment and baseline patient characteristics. Inter-individual variability in the association between treatment exposure and risk of late toxicity suggests that genetic variation possibly modifies this association. We reviewed the available literature on genetic susceptibility of late toxicity after childhood cancer treatment related to components of metabolic syndrome, bone mineral density, gonadal impairment and hearing impairment. Methods: A systematic literature search was performed, using Embase, Cochrane Library, Google Scholar, MEDLINE, and Web of Science databases. Eligible publications included all English language reports of candidate gene studies and genome wide association studies (GWAS) that aimed to identify genetic risk factors associated with the four late toxicities, defined as toxicity present after end of treatment. Results: Twenty-seven articles were identified, including 26 candidate gene studies: metabolic syndrome (n = 6); BMD (n = 6); gonadal impairment (n = 2); hearing impairment (n = 12) and one GWAS (metabolic syndrome). Eighty percent of the genetic studies on late toxicity after childhood cancer had relatively small sample sizes (n < 200), leading to insufficient power, and lacked adjustment for multiple comparisons. Only four (4/26 = 15%) candidate gene studies had their findings validated in independent replication cohorts as part of their own report. Conclusion: Genetic susceptibility associations are not consistent or not replicated and therefore, currently no evidence-based recommendations can be made for hearing impairment, gonadal impairment, bone mineral density impairment and metabolic syndrome in CCS. To advance knowledge related to genetic variation influencing late toxicities among CCS, future studies need adequate power, independent cohorts for replication, harmonization of disease outcomes and sample collections, and (international) collaboration.

UR - https://www.scopus.com/pages/publications/85045686172

UR - https://www.ncbi.nlm.nih.gov/pubmed/29759558

U2 - 10.1016/j.critrevonc.2018.04.001

DO - 10.1016/j.critrevonc.2018.04.001

M3 - Review article

C2 - 29759558

SN - 1040-8428

VL - 126

SP - 154

EP - 167

JO - Critical reviews in oncology/hematology

JF - Critical reviews in oncology/hematology

ER -

The influence of genetic variation on late toxicities in childhood cancer survivors: A review

Abstract

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