The relationship between ionizing radiation-induced apoptosis and stem cells in the small and large intestine

Potten, Christopher S; Grant, Hannah

doi:10.1038/bjc.1998.618

Cited by 217 publications

(158 citation statements)

References 30 publications

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“…Disruption of this balance underlies the development of cancer (Williams, 1991). In the colonic crypt, stem cells are located at the base and as they differentiate they progress up the crypt, eventually dying by apoptosis and are sloughed off into the colonic lumen (Potten and Grant, 1998). The high incidence of colorectal cancer in Western society has been attributed to a diet high in saturated fat and low in dietary fibre (Sandler et al, 1993).…”

Section: Discussionmentioning

confidence: 99%

Opposing effects of butyrate and bile acids on apoptosis of human colon adenoma cells: differential activation of PKC and MAP kinases

et al. 2003

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Butyrate, produced in the colon by fermentation of dietary fibre, induces apoptosis in colon adenoma and cancer cell lines, which may contribute to protection against colorectal cancer. However, butyrate is present in the colon along with other dietary factors, including unconjugated bile acids, which are tumour promoters. We have shown previously that the proapoptotic effects of butyrate on AA/C1 human adenoma cells were reduced in the presence of bile acids. To determine the cellular basis of this interaction, we examined the effects of butyrate and the secondary bile acid ursodeoxycholic acid (UDCA) on signalling pathways known to regulate apoptosis using AA/C1 cells. Butyrate activated PKC-d and p38 MAP (mitogen-activated protein) kinase, whereas UDCA activated PKC-a and p42/44 MAP kinase. Butyrate treatment also resulted in the caspase-3-mediated proteolysis of PKC-d. Butyrate-induced apoptosis was reduced by inhibitors of PKC-d (Rottlerin), p38 MAP kinase (SB202190) and caspase 3 (DEVD-fmk), whereas the proliferative/survival effects of UDCA were blocked by inhibitors of PKC-a (Gö 6976) and MEK 1 (PD98059). The effects of butyrate and bile acids are therefore mediated by the differential activation of signalling pathways that are known to regulate apoptosis.

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Section: Discussionmentioning

confidence: 99%

Opposing effects of butyrate and bile acids on apoptosis of human colon adenoma cells: differential activation of PKC and MAP kinases

et al. 2003

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“…9 Inadequate apoptotic deletion could thus allow development of mutated clones with the potential to progress to cancer. 13,14 Proapoptotic chemopreventive agents might have the opposite effect and, thus, reduce the mutational load resulting from carcinogen exposure.Apart from AARGC, apoptosis occurs in several other contexts of relevance to CRC, including occasional ''spontaneous'' apoptosis in the proliferative zone of normal colonic crypts 15,16 and quite frequent apoptosis occurring in many cancers. 17 The role of p53 in triggering apoptosis in each of these contexts is unclear.…”

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confidence: 99%

mentioning

confidence: 99%

Absence of acute apoptotic response to genotoxic carcinogens in p53‐deficient mice is associated with increased susceptibility to azoxymethane‐induced colon tumours

Ying

Leu

Young

2005

Intl Journal of Cancer

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Acute apoptotic response to genotoxic carcinogens (AARGC) might be important for controlling the consequences of mutational load in the colon. It has been shown to occur in parallel with activation of DNA repair mechanisms. Inadequate AARGC might allow development of mutated clones with the potential to progress to cancer. In this study, we tested if p53 levels were important for AARGC in the colon and whether defective AARGC was associated with increased risk for colorectal oncogenesis. Apoptosis was measured in colonic epithelium of mice from each p53 genotype ( p53 -/-, p53 +/-, wild-type) without and 8 hr following a single injection of azoxymethane (AOM). To determine risk for carcinogen-induced colorectal cancer (CRC), groups of mice from each p53 genotype received 3 weekly injections of AOM and colons were examined for tumour 20 weeks later. Rates of spontaneous apoptosis in colon were not affected by p53 level. However, AARGC was absent in p53 -/-mice and reduced by 50% in p53 +/-mice (both p < 0.01) compared to wild-type mice. AOM induced tumours in 30% of wild-type mice (average multiplicity 1.0 tumours/mouse) compared to 72% of p53 +/-mice (2.0 tumours/ mouse, p < 0.01) and 100% of p53 -/-mice (2.8 tumours/mouse, p < 0.01). Without AOM, significantly fewer mice in all groups had tumours. Rates of apoptosis in tumours were independent of p53 status. p53 dysfunction puts intestinal epithelia at increased risk of genotoxin-induced oncogenesis due to impairment of apoptotic response mechanisms. p53 levels do not appear, however, to be important for spontaneous apoptosis in normal epithelium or apoptosis in tumours. Subsequent studies are now warranted to test the converse, namely, that enhanced apoptotic response to carcinogen reduces risk for colorectal oncogenesis. ' 2005 Wiley-Liss, Inc.Key words: apoptosis; carcinogen; intestinal epithelia; colorectal cancer; p53Clinical and animal studies indicate that CRC development is characterized by progressive genomic instability with multiple genetic alterations. p53 is commonly affected as >50% of CRCs show abnormality in both alleles. p53 plays an important role by recognizing DNA damage, triggering repair and apoptosis and inducing cell cycle arrest. It maintains genomic stability and prevents accumulation of multiple genetic changes characteristic of the development of neoplasia. 1 Attenuated apoptosis and accelerated tumour growth correlate with loss of p53, suggesting that loss of p53-mediated apoptosis is the rate-limiting step in tumour progression. 2,3 Whether p53 is important in regulating genetic events early in oncogenesis, such as initiating mutations, is unclear.Genotoxic carcinogens such as AOM are colorectum-selective carcinogens in rodents that alkylate DNA and initiate oncogenesis by forming DNA adducts. 4 Initiating events such as these may be relevant for humans as mutations consistent with alkylating genotoxin-induced damage have been described in human gastrointestinal tissues 5 and specifically in K-ras and p53. [6][7][8] In response to ...

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“…Epithelial cells are derived from mitotic cells situated in the crypt base (Cheng and Leblond, 1974;Potten, 1998;Potten and Grant, 1998;Wilson et al, 1998); these cells migrate upward to the villi and reach to the top of the villi, where they are extruded into the intestinal lumen within 48-96 hr (Imondi and Bird, 1966;Potten, 1998). This cell turn over seems to induce many types of cell morphologies on the villus apical surface depending upon intestinal function.…”

Section: Discussionmentioning

confidence: 99%

The relationship between intestinal histology and function as shown by compensatory enlargement of remnant villi after midgut resection in chickens

Yamauchi

Incharoen

Yamauchi

2010

The Anatomical Record

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To demonstrate the relationship between intestinal histology and function, we investigated the possibility that compensatory enlargement of villi in the chickens' remnant intestine can be induced after 50% or 80% jejunal resection as well as after 50% jejunal plus 70% ileal resection. Compared with intact control chickens, operated chickens showed an almost similar body weight, nitrogen retention, and ether extract digestibility, an improved dry matter digestibility, and a much greater absorption of protein and ether extract by the remnant jejunum and ileum. This suggests an enhanced absorptive function of the remnant intestine. In these chickens, increased value of most light microscopic parameters, increased frequency of anastomosing of each villus, and increased number of protuberated epithelial cells appeared with an increase in the intestinal resection area. This suggests that intestinal villi and epithelial cells are hypertrophied in the remnant jejunum and ileum, and that intestinal villi adapt to activated intestinal absorptive function not by increasing their numbers, but by fusing together into larger villi. These findings demonstrate that intestinal histology is intimately related to intestinal function.

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The relationship between ionizing radiation-induced apoptosis and stem cells in the small and large intestine

Cited by 217 publications

References 30 publications

Opposing effects of butyrate and bile acids on apoptosis of human colon adenoma cells: differential activation of PKC and MAP kinases

Opposing effects of butyrate and bile acids on apoptosis of human colon adenoma cells: differential activation of PKC and MAP kinases

Absence of acute apoptotic response to genotoxic carcinogens in p53‐deficient mice is associated with increased susceptibility to azoxymethane‐induced colon tumours

The relationship between intestinal histology and function as shown by compensatory enlargement of remnant villi after midgut resection in chickens

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