Severe Hepatopathy in National Wilms Tumor Studies 3-5: Prevalence, Clinical Features, and Outcomes after Reintroduction of Chemotherapy

Natanja Oosterom; Saskia L.M. Gooskens; Lindsay A. Renfro; Elizabeth J. Perlman; Marry M. Van Den Heuvel-Eibrink; Thomas E. Hamilton; Daniel M. Green; Paul E. Grundy; Najat C. Daw; James I. Geller; Jeffrey S. Dome; Conrad V. Fernandez; Elizabeth A. Mullen

doi:10.1200/JCO.22.02555

Severe Hepatopathy in National Wilms Tumor Studies 3-5: Prevalence, Clinical Features, and Outcomes after Reintroduction of Chemotherapy

Natanja Oosterom, Saskia L.M. Gooskens, Lindsay A. Renfro, Elizabeth J. Perlman, Marry M. Van Den Heuvel-Eibrink, Thomas E. Hamilton, Daniel M. Green, Paul E. Grundy, Najat C. Daw, James I. Geller, Jeffrey S. Dome, Conrad V. Fernandez, Elizabeth A. Mullen

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Abstract

PURPOSEThe safety of reintroducing chemotherapy in the pediatric renal tumor setting after severe hepatopathy (SH), including sinusoidal obstruction syndrome (SOS), is uncertain. We describe the incidence, severity, outcomes, and impact on subsequent treatment for patients with SH from National Wilms Tumor Study (NWTS) protocols 3-5.PATIENTS AND METHODSArchived charts for patients enrolled on NWTS 3-5 who met study inclusion criteria for SH by using established hepatopathy grading scales and clinical criteria were reviewed for demographics, tumor characteristics, radio- and chemotherapy details, SH-related dose modifications, and oncologic outcomes. Genomic analysis for candidate polymorphisms associated with SH was performed in 14 patients.RESULTSSeventy-one of 8,862 patients (0.8%) met study inclusion criteria. The median time from therapy initiation to SH was 51 days (range, 2-293 days). Sixty percent received radiotherapy, and 56% had right-sided tumors. Grade 1-4 thrombocytopenia was noted in 70% at initial occurrence of SH (median 22,000/microliter). Among 69 of 71 children with SH occurring before the end of therapy (EOT) and post-SH treatment information available, chemotherapy was delayed posthepatopathy for 65% (69% of these at a reduced dose), continued without delay for 20% (57% of these at reduced dose), and stopped completely for 15% (4 of 10 of whom died of SH). Overall, 42% of patients with dose reductions achieved full dose by EOT. The five-year post-SH event-free survival for patients who continued therapy was 89% (95% CI, 81 to 98), with no significant differences by whether delay or dose reduction occurred. We identified no SH-associated pharmacogenomic polymorphism.CONCLUSIONThe incidence of SH on NWTS 3-5 was low; many had associated severe thrombocytopenia. Careful reintroduction of chemotherapy appeared to be feasible for the majority of patients who developed severe chemotherapy- and/or radiotherapy-induced liver toxicity.

Original language	English (US)
Pages (from-to)	4247-4256
Number of pages	10
Journal	Journal of Clinical Oncology
Volume	41
Issue number	26
DOIs	https://doi.org/10.1200/JCO.22.02555
State	Published - Sep 10 2023
Externally published	Yes

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1200/JCO.22.02555

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Oosterom, N., Gooskens, S. L. M., Renfro, L. A., Perlman, E. J., Van Den Heuvel-Eibrink, M. M., Hamilton, T. E., Green, D. M., Grundy, P. E., Daw, N. C., Geller, J. I., Dome, J. S., Fernandez, C. V., & Mullen, E. A. (2023). Severe Hepatopathy in National Wilms Tumor Studies 3-5: Prevalence, Clinical Features, and Outcomes after Reintroduction of Chemotherapy. Journal of Clinical Oncology, 41(26), 4247-4256. https://doi.org/10.1200/JCO.22.02555

Oosterom, N, Gooskens, SLM, Renfro, LA, Perlman, EJ, Van Den Heuvel-Eibrink, MM, Hamilton, TE, Green, DM, Grundy, PE, Daw, NC, Geller, JI, Dome, JS, Fernandez, CV & Mullen, EA 2023, 'Severe Hepatopathy in National Wilms Tumor Studies 3-5: Prevalence, Clinical Features, and Outcomes after Reintroduction of Chemotherapy', Journal of Clinical Oncology, vol. 41, no. 26, pp. 4247-4256. https://doi.org/10.1200/JCO.22.02555

@article{d04fc76bf45a45918361fbaeb5445f8c,

title = "Severe Hepatopathy in National Wilms Tumor Studies 3-5: Prevalence, Clinical Features, and Outcomes after Reintroduction of Chemotherapy",

abstract = "PURPOSEThe safety of reintroducing chemotherapy in the pediatric renal tumor setting after severe hepatopathy (SH), including sinusoidal obstruction syndrome (SOS), is uncertain. We describe the incidence, severity, outcomes, and impact on subsequent treatment for patients with SH from National Wilms Tumor Study (NWTS) protocols 3-5.PATIENTS AND METHODSArchived charts for patients enrolled on NWTS 3-5 who met study inclusion criteria for SH by using established hepatopathy grading scales and clinical criteria were reviewed for demographics, tumor characteristics, radio- and chemotherapy details, SH-related dose modifications, and oncologic outcomes. Genomic analysis for candidate polymorphisms associated with SH was performed in 14 patients.RESULTSSeventy-one of 8,862 patients (0.8%) met study inclusion criteria. The median time from therapy initiation to SH was 51 days (range, 2-293 days). Sixty percent received radiotherapy, and 56% had right-sided tumors. Grade 1-4 thrombocytopenia was noted in 70% at initial occurrence of SH (median 22,000/microliter). Among 69 of 71 children with SH occurring before the end of therapy (EOT) and post-SH treatment information available, chemotherapy was delayed posthepatopathy for 65% (69% of these at a reduced dose), continued without delay for 20% (57% of these at reduced dose), and stopped completely for 15% (4 of 10 of whom died of SH). Overall, 42% of patients with dose reductions achieved full dose by EOT. The five-year post-SH event-free survival for patients who continued therapy was 89% (95% CI, 81 to 98), with no significant differences by whether delay or dose reduction occurred. We identified no SH-associated pharmacogenomic polymorphism.CONCLUSIONThe incidence of SH on NWTS 3-5 was low; many had associated severe thrombocytopenia. Careful reintroduction of chemotherapy appeared to be feasible for the majority of patients who developed severe chemotherapy- and/or radiotherapy-induced liver toxicity.",

author = "Natanja Oosterom and Gooskens, {Saskia L.M.} and Renfro, {Lindsay A.} and Perlman, {Elizabeth J.} and {Van Den Heuvel-Eibrink}, {Marry M.} and Hamilton, {Thomas E.} and Green, {Daniel M.} and Grundy, {Paul E.} and Daw, {Najat C.} and Geller, {James I.} and Dome, {Jeffrey S.} and Fernandez, {Conrad V.} and Mullen, {Elizabeth A.}",

note = "Publisher Copyright: {\textcopyright} American Society of Clinical Oncology.",

year = "2023",

month = sep,

day = "10",

doi = "10.1200/JCO.22.02555",

language = "English (US)",

volume = "41",

pages = "4247--4256",

journal = "Journal of Clinical Oncology",

issn = "0732-183X",

publisher = "American Society of Clinical Oncology",

number = "26",

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TY - JOUR

T1 - Severe Hepatopathy in National Wilms Tumor Studies 3-5

T2 - Prevalence, Clinical Features, and Outcomes after Reintroduction of Chemotherapy

AU - Oosterom, Natanja

AU - Gooskens, Saskia L.M.

AU - Renfro, Lindsay A.

AU - Perlman, Elizabeth J.

AU - Van Den Heuvel-Eibrink, Marry M.

AU - Hamilton, Thomas E.

AU - Green, Daniel M.

AU - Grundy, Paul E.

AU - Daw, Najat C.

AU - Geller, James I.

AU - Dome, Jeffrey S.

AU - Fernandez, Conrad V.

AU - Mullen, Elizabeth A.

PY - 2023/9/10

Y1 - 2023/9/10

N2 - PURPOSEThe safety of reintroducing chemotherapy in the pediatric renal tumor setting after severe hepatopathy (SH), including sinusoidal obstruction syndrome (SOS), is uncertain. We describe the incidence, severity, outcomes, and impact on subsequent treatment for patients with SH from National Wilms Tumor Study (NWTS) protocols 3-5.PATIENTS AND METHODSArchived charts for patients enrolled on NWTS 3-5 who met study inclusion criteria for SH by using established hepatopathy grading scales and clinical criteria were reviewed for demographics, tumor characteristics, radio- and chemotherapy details, SH-related dose modifications, and oncologic outcomes. Genomic analysis for candidate polymorphisms associated with SH was performed in 14 patients.RESULTSSeventy-one of 8,862 patients (0.8%) met study inclusion criteria. The median time from therapy initiation to SH was 51 days (range, 2-293 days). Sixty percent received radiotherapy, and 56% had right-sided tumors. Grade 1-4 thrombocytopenia was noted in 70% at initial occurrence of SH (median 22,000/microliter). Among 69 of 71 children with SH occurring before the end of therapy (EOT) and post-SH treatment information available, chemotherapy was delayed posthepatopathy for 65% (69% of these at a reduced dose), continued without delay for 20% (57% of these at reduced dose), and stopped completely for 15% (4 of 10 of whom died of SH). Overall, 42% of patients with dose reductions achieved full dose by EOT. The five-year post-SH event-free survival for patients who continued therapy was 89% (95% CI, 81 to 98), with no significant differences by whether delay or dose reduction occurred. We identified no SH-associated pharmacogenomic polymorphism.CONCLUSIONThe incidence of SH on NWTS 3-5 was low; many had associated severe thrombocytopenia. Careful reintroduction of chemotherapy appeared to be feasible for the majority of patients who developed severe chemotherapy- and/or radiotherapy-induced liver toxicity.

AB - PURPOSEThe safety of reintroducing chemotherapy in the pediatric renal tumor setting after severe hepatopathy (SH), including sinusoidal obstruction syndrome (SOS), is uncertain. We describe the incidence, severity, outcomes, and impact on subsequent treatment for patients with SH from National Wilms Tumor Study (NWTS) protocols 3-5.PATIENTS AND METHODSArchived charts for patients enrolled on NWTS 3-5 who met study inclusion criteria for SH by using established hepatopathy grading scales and clinical criteria were reviewed for demographics, tumor characteristics, radio- and chemotherapy details, SH-related dose modifications, and oncologic outcomes. Genomic analysis for candidate polymorphisms associated with SH was performed in 14 patients.RESULTSSeventy-one of 8,862 patients (0.8%) met study inclusion criteria. The median time from therapy initiation to SH was 51 days (range, 2-293 days). Sixty percent received radiotherapy, and 56% had right-sided tumors. Grade 1-4 thrombocytopenia was noted in 70% at initial occurrence of SH (median 22,000/microliter). Among 69 of 71 children with SH occurring before the end of therapy (EOT) and post-SH treatment information available, chemotherapy was delayed posthepatopathy for 65% (69% of these at a reduced dose), continued without delay for 20% (57% of these at reduced dose), and stopped completely for 15% (4 of 10 of whom died of SH). Overall, 42% of patients with dose reductions achieved full dose by EOT. The five-year post-SH event-free survival for patients who continued therapy was 89% (95% CI, 81 to 98), with no significant differences by whether delay or dose reduction occurred. We identified no SH-associated pharmacogenomic polymorphism.CONCLUSIONThe incidence of SH on NWTS 3-5 was low; many had associated severe thrombocytopenia. Careful reintroduction of chemotherapy appeared to be feasible for the majority of patients who developed severe chemotherapy- and/or radiotherapy-induced liver toxicity.

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Severe Hepatopathy in National Wilms Tumor Studies 3-5: Prevalence, Clinical Features, and Outcomes after Reintroduction of Chemotherapy

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