Lumbar-sacral bone marrow dose modeling for acute hematological toxicity in anal cancer patients treated with concurrent chemo-radiation

  • Pierfrancesco Franco
  • , Riccardo Ragona
  • , Francesca Arcadipane
  • , Massimiliano Mistrangelo
  • , Paola Cassoni
  • , Nadia Rondi
  • , Mario Morino
  • , Patrizia Racca
  • , Umberto Ricardi

Risultato della ricerca: Contributo su rivistaArticolo in rivistapeer review

Abstract

The aim of the study was to model acute hematologic toxicity (HT) and dose to pelvic osseous structures in anal cancer patients treated with definitive chemo-radiation (CT-RT). A total of 53 patients receiving CT-RT were analyzed. Pelvic bone marrow and corresponding subsites were contoured: ilium, lower pelvis and lumbosacral spine (LSBM). Dose-volume histograms points and mean doses were collected. Logistic regression was performed to correlate dosimetric parameters and ≥G3 HT as endpoint. Normal tissue complication probability (NTCP) was evaluated with the Lyman-Kutcher-Burman (LKB) model. Logistic regression showed a significant correlation between LSBM-mean dose and ≥G3 leukopenia (β coefficient 0.122; p = 0.030; 95% CI 0.012–0.233). According to NTCP modeling, the predicted HT probability had the following parameters: TD50: 37.5 Gy, γ50: 1.15, m: 0.347. For node positive patients, TD50: 35.2 Gy, γ50: 2.27, m: 0.176 were found. Node positive patients had significantly higher PBM-V15 (Mean 81.1 vs. 86.7%; p = 0.04), -V20 (Mean 72.7 vs. 79.9%; p = 0.01) and V30 (Mean 50.2 vs. 57.3%; p = 0.03). Patients with a mean LSBM dose >32 Gy had a 1.81 (95% CI 0.81–4.0) relative risk to develop ≥G3 leukopenia. For node positive patients, those risks were 2.67 (95% CI 0.71–10). LKB modeling seems to suggest that LSBM-mean dose should be kept below 32 Gy to minimize ≥G3 HT in anal cancer patients treated with IMRT and concurrent chemotherapy. The contribution of LSBM dose in the development of HT above 25 Gy seems steeper in node positive patients.

Lingua originaleInglese
Numero di articolo137
RivistaMedical Oncology
Volume33
Numero di pubblicazione12
DOI
Stato di pubblicazionePubblicato - 1 dic 2016
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