Literature DB >> 12950390

Intestinal crypt clonogens: a new interpretation of radiation survival curve shape and clonogenic cell number.

S A Roberts1, J H Hendry, C S Potten.   

Abstract

Estimates of the clonogen content (number of microcolony-forming cells) of murine intestinal crypts using microcolony assays show an apparent dependence on the radiation dose used in the assay of clonogen content. Crypt radiation survival curves often show increased curvature beyond that expected on the basis of the conventional linear-quadratic model. A novel form of crypt survival curve shape is proposed based on two contributory mechanisms of crypt killing. Six previously published sets of microcolony data were re-analysed using a dual-kill model, where target cells are killed by two contributory mechanisms, each described by a linear-quadratic function of dose. The data were analysed as two series--high-dose rate and low-dose rate irradiation. The data were fitted to the models using direct maximization of a quasi-likelihood, explicitly allowing for overdispersion. The dual-kill model can reproduce both the apparent dose-dependence of the clonogen estimates and the high-dose curvature of the dose-response curves. For both series of data the model was a significantly better fit to the data than the standard linear-quadratic model, with no evidence of any systematic lack of fit. The parameters of the clonogenic cell component of the model are consistent with other studies that suggest a low clonogen number (somewhat less than five) per crypt. The model implies that there is a secondary mechanism decreasing clonogen survival, and hence increasing clonogen number estimates, at high doses. The mechanisms underlying the modification of the dose-response are unclear, and the implied mechanisms of, for example, slow growth, induced either directly in the surviving cells or indirectly through stromal injury or bystander effects are only speculative. Nevertheless, the model fits the data well, demonstrating that there is greater kill at high doses in these experimental series than would be expected from the conventional linear-quadratic model. This alternative model, or another model with similar behaviour, needs to be considered when analysing in detail and interpreting microcolony data as a function of dose. The implied low number of < or = 5 of these regenerative and relatively radioresistant clonogenic cells is distinct from a similar number of much more radiosensitive precursor stem cells which undergo early apoptosis after doses around 1 Gy.

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Year:  2003        PMID: 12950390      PMCID: PMC6495797          DOI: 10.1046/j.1365-2184.2003.00279.x

Source DB:  PubMed          Journal:  Cell Prolif        ISSN: 0960-7722            Impact factor:   6.831


  37 in total

1.  Endothelial cells and radiation gastrointestinal syndrome.

Authors:  H D Suit; H R Withers
Journal:  Science       Date:  2001-11-16       Impact factor: 47.728

2.  Endothelial cells and radiation gastrointestinal syndrome.

Authors:  J H Hendry; C Booth; C S Potten
Journal:  Science       Date:  2001-11-16       Impact factor: 47.728

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Journal:  Mutat Res       Date:  1993-12       Impact factor: 2.433

5.  Alpha/beta ratios and the cycling status of tissue target cells.

Authors:  J H Hendry; C S Potten
Journal:  Radiother Oncol       Date:  1988-05       Impact factor: 6.280

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Journal:  Radiat Res       Date:  1972-11       Impact factor: 2.841

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Journal:  Br J Radiol       Date:  1983-03       Impact factor: 3.039

8.  Cell death (apoptosis) in the mouse small intestine after low doses: effects of dose-rate, 14.7 MeV neutrons, and 600 MeV (maximum energy) neutrons.

Authors:  J H Hendry; C S Potten; C Chadwick; M Bianchi
Journal:  Int J Radiat Biol Relat Stud Phys Chem Med       Date:  1982-12

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Authors:  H D Thames; H R Withers
Journal:  Br J Radiol       Date:  1980-11       Impact factor: 3.039

10.  Cytosar-U (Ara-C) induced changes in mouse jejunal crypt epithelial kinetics and radiosensitivity to gamma rays and fast neutrons.

Authors:  W R Hanson; D L Boston
Journal:  Int J Radiat Oncol Biol Phys       Date:  1983-04       Impact factor: 7.038

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  11 in total

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2.  Loss of p21Waf1/Cip1/Sdi1 enhances intestinal stem cell survival following radiation injury.

Authors:  Robert J George; Mark A Sturmoski; Randal May; Sripathi M Sureban; Brian K Dieckgraefe; Shrikant Anant; Courtney W Houchen
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3.  The stem cells of small intestinal crypts: where are they?

Authors:  C S Potten; R Gandara; Y R Mahida; M Loeffler; N A Wright
Journal:  Cell Prolif       Date:  2009-09-28       Impact factor: 6.831

4.  Characterizing the Natural History of Acute Radiation Syndrome of the Gastrointestinal Tract: Combining High Mass and Spatial Resolution Using MALDI-FTICR-MSI.

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5.  Dose-dependent uptake of 3'-deoxy-3'-[(18) F]fluorothymidine by the bowel after total-body irradiation.

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Journal:  Mol Imaging Biol       Date:  2014-12       Impact factor: 3.488

6.  Mouse models for colorectal cancer.

Authors:  Baktiar O Karim; David L Huso
Journal:  Am J Cancer Res       Date:  2013-06-20       Impact factor: 6.166

7.  The stem cell population of the human colon crypt: analysis via methylation patterns.

Authors:  Pierre Nicolas; Kyoung-Mee Kim; Darryl Shibata; Simon Tavaré
Journal:  PLoS Comput Biol       Date:  2007-01-02       Impact factor: 4.475

8.  A Role for the PPARgamma in Cancer Therapy.

Authors:  Moray J Campbell; Carsten Carlberg; H Phillip Koeffler
Journal:  PPAR Res       Date:  2008       Impact factor: 4.964

Review 9.  Gastrointestinal neuroendocrine peptides/amines in inflammatory bowel disease.

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Journal:  World J Gastroenterol       Date:  2017-07-28       Impact factor: 5.742

10.  Chemoprevention utility of silibinin and Cdk4 pathway inhibition in Apc(-/+) mice.

Authors:  Baktiar O Karim; Ki-Jong Rhee; Guosheng Liu; Dongfeng Zheng; David L Huso
Journal:  BMC Cancer       Date:  2013-03-27       Impact factor: 4.430

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