Radiobiological basis of SBRT and SRS

Stereotactic body radiation therapy (SBRT) and stereotactic radiosurgery (SRS) have been demonstrated to be highly effective for a variety of tumors. However, the radiobiological principles of SBRT and SRS have not yet been clearly defined. It is well known that newly formed tumor blood vessels are...

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Published inInternational journal of clinical oncology Vol. 19; no. 4; pp. 570 - 578
Main Authors Song, Chang W., Kim, Mi-Sook, Cho, L. Chinsoo, Dusenbery, Kathryn, Sperduto, Paul W.
Format Journal Article
LanguageEnglish
Published Tokyo Springer Japan 01.08.2014
Springer Nature B.V
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Abstract Stereotactic body radiation therapy (SBRT) and stereotactic radiosurgery (SRS) have been demonstrated to be highly effective for a variety of tumors. However, the radiobiological principles of SBRT and SRS have not yet been clearly defined. It is well known that newly formed tumor blood vessels are fragile and extremely sensitive to ionizing radiation. Various lines of evidence indicate that irradiation of tumors with high dose per fraction, i.e. >10 Gy per fraction, not only kills tumor cells but also causes significant damage in tumor vasculatures. Such vascular damage and ensuing deterioration of the intratumor environment then cause ischemic or indirect/secondary tumor cell death within a few days after radiation exposure, indicating that vascular damage plays an important role in the response of tumors to SBRT and SRS. Indications are that the extensive tumor cell death due to the direct effect of radiation on tumor cells and the secondary effect through vascular damage may lead to massive release of tumor-associated antigens and various pro-inflammatory cytokines, thereby triggering an anti-tumor immune response. However, the precise role of immune assault on tumor cells in SBRT and SRS has not yet been clearly defined. The “4 Rs” for conventional fractionated radiotherapy do not include indirect cell death and thus 4 Rs cannot account for the effective tumor control by SBRT and SRS. The linear-quadratic model is for cell death caused by DNA breaks and thus the usefulness of this model for ablative high-dose SBRT and SRS is limited.
AbstractList Stereotactic body radiation therapy (SBRT) and stereotactic radiosurgery (SRS) have been demonstrated to be highly effective for a variety of tumors. However, the radiobiological principles of SBRT and SRS have not yet been clearly defined. It is well known that newly formed tumor blood vessels are fragile and extremely sensitive to ionizing radiation. Various lines of evidence indicate that irradiation of tumors with high dose per fraction, i.e. >10 Gy per fraction, not only kills tumor cells but also causes significant damage in tumor vasculatures. Such vascular damage and ensuing deterioration of the intratumor environment then cause ischemic or indirect/secondary tumor cell death within a few days after radiation exposure, indicating that vascular damage plays an important role in the response of tumors to SBRT and SRS. Indications are that the extensive tumor cell death due to the direct effect of radiation on tumor cells and the secondary effect through vascular damage may lead to massive release of tumor-associated antigens and various pro-inflammatory cytokines, thereby triggering an anti-tumor immune response. However, the precise role of immune assault on tumor cells in SBRT and SRS has not yet been clearly defined. The “4 Rs” for conventional fractionated radiotherapy do not include indirect cell death and thus 4 Rs cannot account for the effective tumor control by SBRT and SRS. The linear-quadratic model is for cell death caused by DNA breaks and thus the usefulness of this model for ablative high-dose SBRT and SRS is limited.
Stereotactic body radiation therapy (SBRT) and stereotactic radiosurgery (SRS) have been demonstrated to be highly effective for a variety of tumors. However, the radiobiological principles of SBRT and SRS have not yet been clearly defined. It is well known that newly formed tumor blood vessels are fragile and extremely sensitive to ionizing radiation. Various lines of evidence indicate that irradiation of tumors with high dose per fraction, i.e. >10 Gy per fraction, not only kills tumor cells but also causes significant damage in tumor vasculatures. Such vascular damage and ensuing deterioration of the intratumor environment then cause ischemic or indirect/secondary tumor cell death within a few days after radiation exposure, indicating that vascular damage plays an important role in the response of tumors to SBRT and SRS. Indications are that the extensive tumor cell death due to the direct effect of radiation on tumor cells and the secondary effect through vascular damage may lead to massive release of tumor-associated antigens and various pro-inflammatory cytokines, thereby triggering an anti-tumor immune response. However, the precise role of immune assault on tumor cells in SBRT and SRS has not yet been clearly defined. The "4 Rs" for conventional fractionated radiotherapy do not include indirect cell death and thus 4 Rs cannot account for the effective tumor control by SBRT and SRS. The linear-quadratic model is for cell death caused by DNA breaks and thus the usefulness of this model for ablative high-dose SBRT and SRS is limited.[PUBLICATION ABSTRACT]
Author Cho, L. Chinsoo
Sperduto, Paul W.
Kim, Mi-Sook
Song, Chang W.
Dusenbery, Kathryn
Author_xml – sequence: 1
  givenname: Chang W.
  surname: Song
  fullname: Song, Chang W.
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  organization: Department of Therapeutic Radiology-Radiation Oncology, University of Minnesota Medical School
– sequence: 2
  givenname: Mi-Sook
  surname: Kim
  fullname: Kim, Mi-Sook
  organization: Department of Radiation Oncology, Korea Institute of Radiological and Medical Science
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  fullname: Cho, L. Chinsoo
  organization: Department of Therapeutic Radiology-Radiation Oncology, University of Minnesota Medical School
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  givenname: Paul W.
  surname: Sperduto
  fullname: Sperduto, Paul W.
  organization: Department of Therapeutic Radiology-Radiation Oncology, University of Minnesota Medical School
BackLink https://www.ncbi.nlm.nih.gov/pubmed/24993673$$D View this record in MEDLINE/PubMed
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ISSN 1341-9625
IngestDate Thu Oct 10 22:15:11 EDT 2024
Thu Sep 12 17:00:49 EDT 2024
Tue Oct 15 23:53:46 EDT 2024
Sat Dec 16 12:00:45 EST 2023
IsPeerReviewed true
IsScholarly true
Issue 4
Keywords Vascular damage
SBRT/SRS
Radiobiology
Language English
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  year: 2014
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PublicationTitle International journal of clinical oncology
PublicationTitleAbbrev Int J Clin Oncol
PublicationTitleAlternate Int J Clin Oncol
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Publisher Springer Japan
Springer Nature B.V
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Snippet Stereotactic body radiation therapy (SBRT) and stereotactic radiosurgery (SRS) have been demonstrated to be highly effective for a variety of tumors. However,...
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SubjectTerms Apoptosis
Apoptosis - radiation effects
Blood Vessels - pathology
Blood Vessels - radiation effects
Cancer
Cancer Research
Dose Fractionation
Humans
Immunity, Innate - radiation effects
Medicine
Medicine & Public Health
Neoplasms - pathology
Neoplasms - radiotherapy
Oncology
Radiation therapy
Radiation, Ionizing
Radiobiology
Radiosurgery - adverse effects
Radiosurgery - methods
Review Article
Surgical Oncology
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Title Radiobiological basis of SBRT and SRS
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