Pretreatment with transforming growth factor beta-3 protects small intestinal stem cells against radiation damage in vivo

Potten, Christopher S; Booth, Dawn; Haley, John D.

doi:10.1038/bjc.1997.249

Cited by 97 publications

(56 citation statements)

References 15 publications

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“…The number of surviving crypts per cross section was determined for each mouse by scoring the number of surviving crypts in at least eight complete, welloriented cross sections and dividing the total by the number of cross sections scored. Because size differences in regenerative crypts may affect the probability that a regenerative crypt will appear in a cross section (38,41) we determined the width of 20 representative crypts for EP2 Ϫ/Ϫ mice and their wild-type littermates in longitudinal sections of proximal jejunum at their widest point in each crypt. We did not find any difference in the size of regenerative crypts in EP2 Ϫ/Ϫ mice compared with wild type after 14 Gy ␥-irradiation (data not shown).…”

Section: Methodsmentioning

confidence: 99%

Prosurvival and antiapoptotic effects of PGE₂in radiation injury are mediated by EP₂receptor in intestine

Houchen

Sturmoski

Anant

et al. 2003

American Journal of Physiology-Gastrointestinal and Liver Physi

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The biological activities of PGE2 are mediated through EP receptors (EP1–EP4), plasma membrane G protein-coupled receptors that differ in ligand binding and signal-transduction pathways. We investigated gastrointestinal EP2 receptor expression in adult mice before and after radiation injury and evaluated intestinal stem cell survival and crypt epithelial apoptosis after radiation injury in EP2 null mice. EP2 was expressed throughout the gut. Intestinal EP2 mRNA increased fivefold after γ-irradiation. Crypt survival was diminished in EP2 −/− mice (4.06 crypts/cross section) compared with wild-type littermates (8.15 crypts/cross section). Radiation-induced apoptosis was significantly increased in EP2 −/− mice compared with wild-type littermates. Apoptosis was 1.6-fold higher in EP2 −/− mice (5.9 apoptotic cells/crypt) than in wild-type mice (3.5 apoptotic cells/crypt). The EP2receptor is expressed in mouse gastrointestinal epithelial cells and is upregulated following radiation injury. The effects of PGE2on both crypt epithelial apoptosis and intestinal crypt stem cell survival are mediated through the EP2 receptor.

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Section: Methodsmentioning

confidence: 99%

Prosurvival and antiapoptotic effects of PGE₂in radiation injury are mediated by EP₂receptor in intestine

Houchen

Sturmoski

Anant

et al. 2003

American Journal of Physiology-Gastrointestinal and Liver Physi

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“…139 TGF-␤ 3 inhibits cell cycle progression through G1. 140 In an animal model for radiation-induced small intestine damage, Potten et al 140 could demonstrate a fourto six-fold increase in survival of small intestinal crypts and a significantly increased survival of animals, if TGF-␤ was administered over a 24 h period prior to irradiation.…”

Section: Transforming Growth Factor Beta (Tgf-␤)mentioning

confidence: 99%

Prophylaxis and treatment of chemo- and radiotherapy-induced oral mucositis – are there new strategies?

Karthaus

Rosenthal

Ganser

1999

Bone Marrow Transplant

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Summary:Oral mucositis is a major dose-limiting toxic effect of intensive cancer chemotherapy. Oral complications may lead to dose reduction or delay in further cancer treatment. Mucositis can be caused directly by cytotoxic effects and indirectly by sustained neutropenia after cytostatic therapy. An impaired mucosal barrier predisposes to life-threatening septic complications during aplasia. The prevalence of an oral focus in febrile neutropenia has been reported in up to 30% of cases and also reduces quality of life. The basic strategies aim at pain relief and prevention of bacterial and fungal infectious complications. However, no effective causal prophylaxis or treatment of oral mucositis is widely accepted. The introduction of cytokines, eg granulocytemacrophage colony-stimulating factor (GM-CSF) and granulocyte colony-stimulating factor (G-CSF) for oral mucositis may be particularly effective and offer a new and hopeful approach. At present, the optimal growth factor, best schedule, effective dosage and best mode of application is not known.

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“…Positive results have been obtained in humans using mouthwashes containing recombinant TGF-b3 (Wymenga et al, 1999), indicating a promising treatment against the oral complications of anti-cancer therapy. Administration of recombinant TGF-b3 directly into the small intestine of mice had a protective effect during radiation (Potten et al, 1997) by reducing stem cell cycling (Booth et al, 2000). To our knowledge however, no study has been done investigating the potential protective effects of orally administrated TGF-b2 originating from a natural source.…”

mentioning

confidence: 99%

Transforming Growth Factor-β2 protects the small intestine during methotrexate treatment in rats possibly by reducing stem cell cycling

Land¹,

Meijer²,

Frerichs³

et al. 2002

Br J Cancer

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During chemo-and radiation therapy, the balance between epithelial cell proliferation, differentiation, and cell death at the villus tip is disrupted by premature death of dividing epithelial cells. This will subsequently lead to the onset of mucosal barrier injury in the whole gastrointestinal tract. Up till now there is no validated method to treat side effects occurring due to therapy. An approach to manage this side effect might be to reversibly arrest growth of epithelial stem cells during therapy using Transforming Growth Factor-b2. A Transforming Growth Factor-b2 enriched fraction prepared from bovine milk was shown to protect small intestinal epithelial cells against cell cycle specific chemotherapeutic agents by arresting the cells in G1-phase. Secondly, in a rat model for induced small intestinal damage, oral supplementation of rats exposed to methotrexate with the Transforming Growth Factor-b2 enriched fraction significantly reduced the chemotherapy-associated weight loss and ileal villus atrophy by reducing cell proliferation in the normal stem cell population. Thus oral supplementation with a bovine milk fraction enriched for Transforming Growth Factor-b2 attenuated the side effects of chemotherapy in the small intestine in rats.

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Pretreatment with transforming growth factor beta-3 protects small intestinal stem cells against radiation damage in vivo

Cited by 97 publications

References 15 publications

Prosurvival and antiapoptotic effects of PGE₂in radiation injury are mediated by EP₂receptor in intestine

Prosurvival and antiapoptotic effects of PGE₂in radiation injury are mediated by EP₂receptor in intestine

Prophylaxis and treatment of chemo- and radiotherapy-induced oral mucositis – are there new strategies?

Transforming Growth Factor-β2 protects the small intestine during methotrexate treatment in rats possibly by reducing stem cell cycling

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Pretreatment with transforming growth factor beta-3 protects small intestinal stem cells against radiation damage in vivo

Cited by 97 publications

References 15 publications

Prosurvival and antiapoptotic effects of PGE2in radiation injury are mediated by EP2receptor in intestine

Prosurvival and antiapoptotic effects of PGE2in radiation injury are mediated by EP2receptor in intestine

Prophylaxis and treatment of chemo- and radiotherapy-induced oral mucositis – are there new strategies?

Transforming Growth Factor-β2 protects the small intestine during methotrexate treatment in rats possibly by reducing stem cell cycling

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Prosurvival and antiapoptotic effects of PGE₂in radiation injury are mediated by EP₂receptor in intestine

Prosurvival and antiapoptotic effects of PGE₂in radiation injury are mediated by EP₂receptor in intestine