Literature DB >> 26520723

Radiotherapy for stage I seminoma of the testis: Organ equivalent dose to partially in-field structures and second cancer risk estimates on the basis of a mechanistic, bell-shaped, and plateau model.

Michalis Mazonakis1, Charalambos Varveris2, Efrossyni Lyraraki2, John Damilakis1.   

Abstract

PURPOSE: The aim of the current study was to (a) calculate the organ equivalent dose (OED) and (b) estimate the associated second cancer risk to partially in-field critical structures from adjuvant radiotherapy for stage I seminoma of the testis on the basis of three different nonlinear risk models.
METHODS: Three-dimensional plans were created for twelve patients who underwent a treatment planning computed tomography of the abdomen. The plans for irradiation of seminoma consisted of para-aortic anteroposterior and posteroanterior fields giving 20 Gy to the target site with 6 MV photons. The OED of stomach, colon, liver, pancreas, and kidneys, that were partially included in the treatment volume, was calculated using differential dose-volume histograms. The mechanistic, bell-shaped, and plateau models were employed for these calculations provided that organ-specific parameters were available for the subsequent assessment of the excess absolute risk (EAR) for second cancer development. The estimated organ-specific lifetime risks were compared with the respective nominal intrinsic probabilities for cancer induction.
RESULTS: The mean OED, which was calculated from the patients' treatment plans, varied from 0.54 to 6.61 Gy by the partially in-field organ of interest and the model used for dosimetric calculations. The difference between the OED of liver derived from the mechanistic model with those from the bell-shaped and plateau models was less than 1.8%. An even smaller deviation of 1.0% was observed for colon. For the rest organs of interest, the differences between the OED values obtained by the examined models varied from 8.6% to 50.0%. The EAR for stomach, colon, liver, pancreas, and kidney cancer induction at an age of 70 yr because of treatment of a typical 39-yr-old individual was up to 4.24, 11.39, 0.91, 3.04, and 0.14 per 10 000 persons-yr, respectively. Patient's irradiation was found to elevate the lifetime intrinsic risks by 8.3%-63.0% depending upon the organ of interest and the model employed for risk analysis.
CONCLUSIONS: Radiotherapy for stage I seminoma of the testis may result in an excess risk for the appearance of secondary malignancies in partially in-field organs. The organ- and model-dependent second cancer risk assessments of this study may be of value for patient counseling and follow-up.

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Year:  2015        PMID: 26520723     DOI: 10.1118/1.4932394

Source DB:  PubMed          Journal:  Med Phys        ISSN: 0094-2405            Impact factor:   4.071


  3 in total

Review 1.  Radiotherapy in testicular germ cell tumours - a literature review.

Authors:  Joanna Jonska-Gmyrek; Piotr Peczkowski; Wojciech Michalski; Grazyna Poniatowska; Agnieszka Zolciak-Siwinska; Beata Kotowicz; Pawel Wiechno; Magdalena Golawska; Maria Kowalska; Tomasz Demkow
Journal:  Contemp Oncol (Pozn)       Date:  2017-09-29

2.  Estimating Second Malignancy Risk in Intensity-Modulated Radiotherapy and Volumetric-Modulated Arc Therapy using a Mechanistic Radiobiological Model in Radiotherapy for Carcinoma of Left Breast.

Authors:  Vasanthan Sakthivel; Ganesh Kadirampatti Mani; Sunil Mani; Raghavendiran Boopathy; Jothybasu Selvaraj
Journal:  J Med Phys       Date:  2017 Oct-Dec

3.  Patients with non-colorectal cancers may be at elevated risk of colorectal neoplasia.

Authors:  Hamzah Abu-Sbeih; Faisal S Ali; Wei Qiao; Phillip Lum; Mehnaz A Shafi; Robert S Bresalier; Ernest Hawk; Gottumukkala S Raju; Yinghong Wang
Journal:  J Cancer       Date:  2020-03-04       Impact factor: 4.207

  3 in total

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