1. The dosimetric impact of axillary nodes contouring variability in breast cancer radiotherapy: An AIRO multi-institutional study
- Author
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Maria Cristina Leonardi, Matteo Pepa, Rosa Luraschi, Sabrina Vigorito, Samantha Dicuonzo, Lars Johannes Isaksson, Maria Rosa La Porta, Lorenza Marino, Edy Ippolito, Alessandra Huscher, Angela Argenone, Fiorenza De Rose, Francesca Cucciarelli, Maria Carmen De Santis, Francesca Rossi, Agnese Prisco, Roberta Guarnaccia, Paola Tabarelli de Fatis, Isabella Palumbo, Sarah Pia Colangione, Maria Mormile, Vincenzo Ravo, Alessandra Fozza, Cynthia Aristei, Roberto Orecchia, Federica Cattani, Barbara Alicja Jereczek-Fossa, Simone Giovanni Gugliandolo, Anna Morra, Marianna Alessandra Gerardi, Maria Alessia Zerella, Domenico Cante, Edoardo Petrucci, Giuseppina Borzì, Maristella Marrocco, Matteo Chieregato, Luciano Iadanza, Francesca Lobefalo, Marco Valenti, Anna Cavallo, Serenella Russo, Marika Guernieri, Tiziana Malatesta, Ilaria Meaglia, Marco Liotta, Marta Marcantonini, Emilio Mezzenga, Sara Falivene, Cecilia Arrichiello, Maria Paola Barbero, Giovanni Battista Ivaldi, Gianpiero Catalano, Cristiana Vidali, Caterina Giannitto, Delia Ciardo, Antonella Ciabattoni, and Icro Meattini
- Subjects
Radiotherapy ,Radiotherapy Planning, Computer-Assisted ,Radiotherapy Planning ,Inter-observer variability ,Radiotherapy Dosage ,Breast Neoplasms ,Hematology ,Nodal contouring ,Breast cancer ,Computer-Assisted ,Oncology ,Dosimetry ,Intensity-Modulated ,Humans ,Female ,Radiology, Nuclear Medicine and imaging ,Lymph Nodes ,Radiotherapy, Intensity-Modulated ,Radiometry - Abstract
To quantify the dosimetric impact of contouring variability of axillary lymph nodes (L2, L3, L4) in breast cancer (BC) locoregional radiotherapy (RT).18 RT centres were asked to plan a locoregional treatment on their own planning target volume (single centre, SC-PTV) which was created by applying their institutional margins to the clinical target volume of the axillary nodes of three BC patients (P1, P2, P3) previously delineated (SC-CTV). The gold standard CTVs (GS-CTVs) of P1, P2 and P3 were developed by BC experts' consensus and validated with STAPLE algorithm. For each participating centre, the GS-PTV of each patient was created by applying the same margins as those used for the SC-CTV to SC-PTV expansion and replaced the SC-PTV in the treatment plan. Datasets were imported into MIM v6.1.7 [MIM Software Inc.], where dose-volume histograms (DVHs) were extracted and differences were analysed.17/18 centres used intensity-modulated RT (IMRT). The CTV to PTV margins ranged from 0 to 10 mm (median 5 mm). No correlation was observed between GS-CTV coverage by 95% isodose and GS-PTV margins width. Doses delivered to 98% (D98) and 95% (D95) of GS-CTVs were significantly lower than those delivered to the SC-CTVs. No significant difference between SC-CTV and GS-CTV was observed in maximum dose (D2), always under 110%. Mean dose ≥99% of the SC-CTVs and GS-CTVs was satisfied in 84% and 50%, respectively. In less than one half of plans, GS-CTV V95% was above 90%. Breaking down the GS-CTV into the three nodal levels (L2, L3 and L4), L4 had the lowest probability to be covered by the 95% isodose.Overall, GS-CTV resulted worse coverage, especially for L4. IMRT was largely used and CTV-to-PTV margins did not compensate for contouring issues. The results highlighted the need for delineation training and standardization.
- Published
- 2022
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