Vozenin-Brotons M. Tissue toxicity induced by ionizing radiation to the normal intestine: Understanding the pathophysiological mechanisms to improve the medical management. World J Gastroenterol 2007; 13(22): 3031-3032 [PMID: 17589916 DOI: 10.3748/wjg.v13.i22.3031]
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MC Vozenin-Brotons, Laboratoire UPRES EA 27-10, “Radiosensibilité des tumeurs et tissus sains”. PR1, 39, Rue Camille Desmoulins, 94805 Villejuif Cedex, France. vozenin@igr.fr
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World J Gastroenterol. Jun 14, 2007; 13(22): 3031-3032 Published online Jun 14, 2007. doi: 10.3748/wjg.v13.i22.3031
Tissue toxicity induced by ionizing radiation to the normal intestine: Understanding the pathophysiological mechanisms to improve the medical management
MC Vozenin-Brotons, UPRES EA 27-10 "Radiosensibilité des tumeurs et tissus sains". Institut de Radioprotection et de Sûreté Nucléaire/Institut Gustave Roussy. Villejuif, France
MC Vozenin-Brotons, Laboratoire de Radiopathologie. SRBE/DRPH. Institut de Radioprotection et de Sûreté Nucléaire. Fontenay-aux-Roses, France
ORCID number: $[AuthorORCIDs]
Author contributions: All authors contributed equally to the work.
Correspondence to: MC Vozenin-Brotons, Laboratoire UPRES EA 27-10, “Radiosensibilité des tumeurs et tissus sains”. PR1, 39, Rue Camille Desmoulins, 94805 Villejuif Cedex, France. vozenin@igr.fr
Telephone: +33-1-42114282 Fax: +33-1-42115236
Received: February 26, 2007 Revised: March 15, 2007 Accepted: March 21, 2007 Published online: June 14, 2007
Abstract
Key Words: $[Keywords]
Citation: Vozenin-Brotons M. Tissue toxicity induced by ionizing radiation to the normal intestine: Understanding the pathophysiological mechanisms to improve the medical management. World J Gastroenterol 2007; 13(22): 3031-3032
At the present time, more than one-half of all cancer patients are treated with radiation therapy. Despite a good therapeutic index, radiotherapy can disable normal tissue injury to normal tissues in long-term cancer survivors. Thus, an important challenge to modern radiation therapy is to increase the tolerance of normal tissues, in order to improve the quality of life of the patients, and to enhance local tumor control using dose escalation and/or new biological radiosensitizers[1]. The recent progress made by 3D-conformal and intensity-modulated radiation therapy has reduced radiation-induced complications especially in dose-limiting organs like the intestine[2]. Yet, acute intestinal complications do occur but are generally transient, whereas low and mild grade chronic gastrointestinal side effects continue to influence the patient’s quality of life. Because the clinical evolution of delayed intestinal toxicity is progressive and inevitable, these complications are of much concern in clinical practice and further improvement in the management of such patients is required.
The current serie published in the World Journal of Gastroenterology contains several articles reviewing the most recent research in the field of radiation-induced intestinal toxicity the current therapeutic advances according to the patient’s symptoms as well as constructive proposals for the improvement of the medical management of such patients. The proposed improvements depend upon the development of reliable diagnostic tests that are able to identify the underlying causes of the symptoms. The contribution by Lutgens et al[3] provides evidence that citrullinemia can be used in clinical and experimental settings as a biomaker of epithelial cell loss. The review by Kruse et al[4] addresses the recent advances in the use of micro array for the prediction of radiosensitivity and damage to normal tissues as well as their main limitations.
The physiopathological, cellular and molecular mechanisms of radiation-induced toxicity have been discussed according to the cellular compartments of the intestine and their implication to acute and chronic intestinal toxicity. Tissue exposure to ionizing radiation stimulates the local production of reactive oxygen species which induce replicative and apoptotic death of epithelial and microvascular endothelial cells of the intestinal mucosa. However, the intestinal response to radiation injury cannot be restricted to a simple cell-killing process but depends upon continuous and integrated pathogenic processes involving cell differentiation and crosstalk between the various cellular components within the extracellular matrix. Otterson[5] reviews the impact of irradiation on gastrointestinal motility with special emphasis on the enteric nervous system. Molla et al[6], Wang et al[7] discuss the role of radiation-induced vascular damage in the acute and delayed intestinal response to ionizing radiation. The radiation-induced alterations of intracellular signaling pathways lead to the transactivation of specific target genes such as genes coding for paracrine factors including vasoactive factors, thrombogenic agents, pro/anti inflammatory mediators and growth factors. The review by Verrechia et al[8] focuses on the role of TGF-β1 in fibrogenesis. TGF-β1 is a potent fibrogenic growth factor that triggers alterations in the resident cell phenotypes that subsequently modify cell to cell interactions and tissue composition. Finally, the extracellular matrix itself may contribute to the self-perpetuation of these wound healing signals by the release of growth factors and by constant activation of cell phenotype via membrane-associated receptors. The long-term persistence of these phenotypical alterations may have an impact on the activity of neighboring cells (mesenchymal, endothelial, epithelial or immune cells) and may lead to a possible amplification of the wound healing signals that perpetuate fibrosis. This aspect has been well discussed by Haydont et al[9].
It is clear from these articles that the normal intestinal response to radiation injury cannot be restricted to a simple cell-killing process. Therefore, the previous concept of a primary cell target in which a single-cell type (whether it is epithelial or endothelial cell) dictated the whole tissue response to radiation injury should be replaced by the concept of coordinated multicellular response that may lead to either tissue recovery or to the development of complications[10]. The recent advances in this field should lead in the near future to the development of biologically-based therapeutic strategies which can be used clinical practice. These strategies would also be applicable to treat radiation injury in the event of radiation accidents or acts of terrorism and would help to improve the therapeutic management of other chronic intestinal diseases.
Footnotes
S- Editor Wang J L- Editor Anand BS E- Editor Ma WH
Lutgens L, Lambin P. Biomarkers for radiation-induced small bowel epithelial damage: An emerging role for plasma Citrulline.World J Gastroenterol. 2007;13:3033-3042.
[PubMed] [DOI][Cited in This Article: ]
Kruse JJ, Stewart FA. Gene expression arrays as a tool to unravel mechanisms of normal tissue radiation injury and prediction of response.World J Gastroenterol. 2007;13:2669-2674.
[PubMed] [DOI][Cited in This Article: ]
Wang J, Boerma M, Fu Q, Hauer-Jensen M. Significance of endothelial dysfunction in the pathogenesis of early and delayed radiation enteropathy.World J Gastroenterol. 2007;13:3047-3055.
[PubMed] [DOI][Cited in This Article: ]
