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Wilms’ tumor
- Glossary
Children’s Oncology Group (COG) histologic classification (1)
Favorable histology Wilms’ tumor
- No evidence of anaplasia
Un-favorable histology Wilms’ tumor
a. Focal anaplastic Wilms’ tumor
- Anaplasia confined to one or more discrete sites within the primary tumor with no extrarenal involvement
- No nuclear unrest outside anaplastic foci
b. Diffuse anaplastic Wilms’ tumor
- Non-localized anaplasia
- Anaplasia in invasive sites or extrarenal deposits
- Localized anaplasia with severe nuclear unrest
- Anaplasia in a random biopsy specimen
- Anaplasia involving the edge of one or more sections.
Blastemal predominant histology (post chemotherapy) (2)
▪️ Presence of residual undifferentiated blastemal cells of over 66% in a tumour with more than 33% of cells viable after preoperative chemotherapy.
Risk group definition for patients with favorable histology WT (3)
Low risk:
▪️ Stages I-II.
Standard risk:
▪️ Stage III.
▪️ Stage IV (pulmonary metastasis only) and RCR post week 6.
High risk:
▪️ Stage IV (pulmonary metastasis only) with SIR post week 6.
▪️ Stage IV (extra pulmonary metastasis).
Response criteria for stage IV favorable histology with pulmonary metastasis: (4)
Rapid complete responder (RCR): complete resolution of pulmonary metastases after 6 weeks of pre-nephrectomy chemotherapy with vincristine, dactinomycin, and doxorubicin.
Slow incomplete responder (SIR): incomplete resolution of pulmonary metastases after 6 weeks of pre-nephrectomy chemotherapy with vincristine, dactinomycin, and doxorubicin.
Risk stratification at relapse definitions: (5)
- Standard risk: patients with initial stage I−II low-risk or intermediate-risk tumours, who received only vincristine and/or actinomycin D (no radiotherapy) in their first-line treatment.
- High risk: Patients without initial diffuse anaplasia or blastemal-type histology, who have already received doxorubicin in their initial treatment.
- Very high risk: Patients with recurrent anaplastic or blastemal-predominant tumor.
