Tumor control probability for selective boosting of hypoxic subvolumes, including the effect of reoxygenation

Tumor control probability for selective boosting of hypoxic subvolumes, including the effect of reoxygenation

To study the effect on tumor control probability of selectively boosting the dose to hypoxic subvolumes. A Monte Carlo model was developed that separates the tumor into two compartments, one of which receives a primary dose, and one of which receives a higher boost dose. During radiation delivery, e...

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Bibliographic Details
Published in:International journal of radiation oncology, biology, physics Vol. 54; no. 3; p. 921
Main Authors: Popple, Richard A, Ove, Roger, Shen, Sui
Format: Journal Article
Language:English
Published: United States 01-11-2002
Subjects:
Algorithms
Cell Hypoxia - physiology
Humans
Monte Carlo Method
Neoplasms - pathology
Neoplasms - physiopathology
Neoplasms - radiotherapy
Oxygen - administration & dosage
Radiation Tolerance - physiology
Radiotherapy Dosage
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Summary:To study the effect on tumor control probability of selectively boosting the dose to hypoxic subvolumes. A Monte Carlo model was developed that separates the tumor into two compartments, one of which receives a primary dose, and one of which receives a higher boost dose. During radiation delivery, each compartment consists of three clonogen subpopulations: those that are well oxygenated, those that are temporarily hypoxic (geometrically transient hypoxia), and those that are permanently hypoxic (geometrically stable hypoxia). The spatial location of temporary hypoxia within the tumor volume varies over time, whereas, the spatial location of permanent hypoxia does not. The effect of reoxygenation was included. Clonogen proliferation was not included in the model. A modest boost dose (120%-150% of the primary dose) increases tumor control probability to that found in the absence of permanent hypoxia. The entire hypoxic subvolume need not be included to obtain a significant benefit. However, only tumors with a geometrically stable hypoxic volume will have an improved control rate. Tumors with an identifiable geometrically stable hypoxic volume will have an improved control rate if the dose to the hypoxic volume is escalated. Further work is required to determine the spatiotemporal evolution of the hypoxic volumes before and during the course of radiotherapy.
ISSN:0360-3016
DOI:10.1016/S0360-3016(02)03007-9