Association of stem-like cells in gender-specific chemoprevention against intestinal neoplasia in MIN mouse

Seema R. Gandhi; Ashish K. Tiwari; Dhananjay P. Kunte; Mart Angelo De La Cruz; Yolanda Stypula; Tina Gibson; Jeffrey Brasky; Vadim Backman; Ramesh K. Wali; Hemant K. Roy

doi:10.3892/or.2011.1395

Association of stem-like cells in gender-specific chemoprevention against intestinal neoplasia in MIN mouse

Seema R. Gandhi, Ashish K. Tiwari, Dhananjay P. Kunte, Mart Angelo De La Cruz, Yolanda Stypula, Tina Gibson, Jeffrey Brasky, Vadim Backman, Ramesh K. Wali^*, Hemant K. Roy

^*Corresponding author for this work

Biomedical Engineering

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Abstract

This study was undertaken to examine the gender-sensitivity and chemopreventive responsiveness of celecoxib on intestinal stem-like cells as a biomarker of colon carcino-genesis, using the MIN mouse model. Male and female MIN mice (6-7-weeks old) were randomized to either control diet or to a diet supplemented with celecoxib (1,500 ppm). The animals were euthanized ten weeks later and the intestines were flushed and opened longitudinally to assess tumor count. Small intestinal segments were formalin-fixed and tissue sections were subjected to immunohistochemical evaluation of DCAMKL1, a known marker of stem-like cells. We found that in animals receiving control (AIN 76A diet) alone, female MIN mice had a higher polyp count than males (52.32±13.89 vs. 35.43±16.05; p<0.0005). However, compared to control diet groups, celecoxib supplementation caused a larger reduction in the number of polyps in females than their male cohorts (6.38±1.43 vs. 12.83±6.74; a reduction of 88% in females to 64% in males). Significant differences (p=0.013) were observed in the number of DCAMKL1-stained cells in the crypts of the wild-type (WT) (10.01±1.07 stem cells per high powered field; HPF) compared to the MIN mice (24.15±8.08 stem cells per HPF), illustrating increased stem-like cells in animals that are more prone to neoplasia. DCAMKL1 labeled stem-like cells were equal in number in the male and female groups receiving the control AIN 76A diet alone (females, 25.73 stem-like cells/HPF); males, 24.15 stem-like cells/HPF). However, females showed a greater reduction in the number of DCAMKL1-labeled stem-like cells with celecoxib supplementation than the respective males (16.63±4.23 vs. 21.56±9.06; a reduction of 35.4% in females to 10.7% in males). We conclude that a higher number of stem-like cells in the uninvolved mucosa paralleled tumorigenesis and mirrored greater chemopreventive responsiveness of female MIN mice compared to males.

Original language	English (US)
Pages (from-to)	1127-1132
Number of pages	6
Journal	Oncology reports
Volume	26
Issue number	5
DOIs	https://doi.org/10.3892/or.2011.1395
State	Published - Nov 2011

Keywords

Celecoxib
Chemoprevention
Doublecortin and calcium/calmodulin- dependent protein kinase-like-1
Gender
Intestine
Stem-like cells

ASJC Scopus subject areas

Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3892/or.2011.1395

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@article{52cf4e3a181245689d9382761c28deb1,

title = "Association of stem-like cells in gender-specific chemoprevention against intestinal neoplasia in MIN mouse",

abstract = "This study was undertaken to examine the gender-sensitivity and chemopreventive responsiveness of celecoxib on intestinal stem-like cells as a biomarker of colon carcino-genesis, using the MIN mouse model. Male and female MIN mice (6-7-weeks old) were randomized to either control diet or to a diet supplemented with celecoxib (1,500 ppm). The animals were euthanized ten weeks later and the intestines were flushed and opened longitudinally to assess tumor count. Small intestinal segments were formalin-fixed and tissue sections were subjected to immunohistochemical evaluation of DCAMKL1, a known marker of stem-like cells. We found that in animals receiving control (AIN 76A diet) alone, female MIN mice had a higher polyp count than males (52.32±13.89 vs. 35.43±16.05; p<0.0005). However, compared to control diet groups, celecoxib supplementation caused a larger reduction in the number of polyps in females than their male cohorts (6.38±1.43 vs. 12.83±6.74; a reduction of 88% in females to 64% in males). Significant differences (p=0.013) were observed in the number of DCAMKL1-stained cells in the crypts of the wild-type (WT) (10.01±1.07 stem cells per high powered field; HPF) compared to the MIN mice (24.15±8.08 stem cells per HPF), illustrating increased stem-like cells in animals that are more prone to neoplasia. DCAMKL1 labeled stem-like cells were equal in number in the male and female groups receiving the control AIN 76A diet alone (females, 25.73 stem-like cells/HPF); males, 24.15 stem-like cells/HPF). However, females showed a greater reduction in the number of DCAMKL1-labeled stem-like cells with celecoxib supplementation than the respective males (16.63±4.23 vs. 21.56±9.06; a reduction of 35.4% in females to 10.7% in males). We conclude that a higher number of stem-like cells in the uninvolved mucosa paralleled tumorigenesis and mirrored greater chemopreventive responsiveness of female MIN mice compared to males.",

keywords = "Celecoxib, Chemoprevention, Doublecortin and calcium/calmodulin- dependent protein kinase-like-1, Gender, Intestine, Stem-like cells",

author = "Gandhi, {Seema R.} and Tiwari, {Ashish K.} and Kunte, {Dhananjay P.} and {De La Cruz}, {Mart Angelo} and Yolanda Stypula and Tina Gibson and Jeffrey Brasky and Vadim Backman and Wali, {Ramesh K.} and Roy, {Hemant K.}",

year = "2011",

month = nov,

doi = "10.3892/or.2011.1395",

language = "English (US)",

volume = "26",

pages = "1127--1132",

journal = "Oncology Reports",

issn = "1021-335X",

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T1 - Association of stem-like cells in gender-specific chemoprevention against intestinal neoplasia in MIN mouse

AU - Gandhi, Seema R.

AU - Tiwari, Ashish K.

AU - Kunte, Dhananjay P.

AU - De La Cruz, Mart Angelo

AU - Stypula, Yolanda

AU - Gibson, Tina

AU - Brasky, Jeffrey

AU - Backman, Vadim

AU - Wali, Ramesh K.

AU - Roy, Hemant K.

PY - 2011/11

Y1 - 2011/11

N2 - This study was undertaken to examine the gender-sensitivity and chemopreventive responsiveness of celecoxib on intestinal stem-like cells as a biomarker of colon carcino-genesis, using the MIN mouse model. Male and female MIN mice (6-7-weeks old) were randomized to either control diet or to a diet supplemented with celecoxib (1,500 ppm). The animals were euthanized ten weeks later and the intestines were flushed and opened longitudinally to assess tumor count. Small intestinal segments were formalin-fixed and tissue sections were subjected to immunohistochemical evaluation of DCAMKL1, a known marker of stem-like cells. We found that in animals receiving control (AIN 76A diet) alone, female MIN mice had a higher polyp count than males (52.32±13.89 vs. 35.43±16.05; p<0.0005). However, compared to control diet groups, celecoxib supplementation caused a larger reduction in the number of polyps in females than their male cohorts (6.38±1.43 vs. 12.83±6.74; a reduction of 88% in females to 64% in males). Significant differences (p=0.013) were observed in the number of DCAMKL1-stained cells in the crypts of the wild-type (WT) (10.01±1.07 stem cells per high powered field; HPF) compared to the MIN mice (24.15±8.08 stem cells per HPF), illustrating increased stem-like cells in animals that are more prone to neoplasia. DCAMKL1 labeled stem-like cells were equal in number in the male and female groups receiving the control AIN 76A diet alone (females, 25.73 stem-like cells/HPF); males, 24.15 stem-like cells/HPF). However, females showed a greater reduction in the number of DCAMKL1-labeled stem-like cells with celecoxib supplementation than the respective males (16.63±4.23 vs. 21.56±9.06; a reduction of 35.4% in females to 10.7% in males). We conclude that a higher number of stem-like cells in the uninvolved mucosa paralleled tumorigenesis and mirrored greater chemopreventive responsiveness of female MIN mice compared to males.

AB - This study was undertaken to examine the gender-sensitivity and chemopreventive responsiveness of celecoxib on intestinal stem-like cells as a biomarker of colon carcino-genesis, using the MIN mouse model. Male and female MIN mice (6-7-weeks old) were randomized to either control diet or to a diet supplemented with celecoxib (1,500 ppm). The animals were euthanized ten weeks later and the intestines were flushed and opened longitudinally to assess tumor count. Small intestinal segments were formalin-fixed and tissue sections were subjected to immunohistochemical evaluation of DCAMKL1, a known marker of stem-like cells. We found that in animals receiving control (AIN 76A diet) alone, female MIN mice had a higher polyp count than males (52.32±13.89 vs. 35.43±16.05; p<0.0005). However, compared to control diet groups, celecoxib supplementation caused a larger reduction in the number of polyps in females than their male cohorts (6.38±1.43 vs. 12.83±6.74; a reduction of 88% in females to 64% in males). Significant differences (p=0.013) were observed in the number of DCAMKL1-stained cells in the crypts of the wild-type (WT) (10.01±1.07 stem cells per high powered field; HPF) compared to the MIN mice (24.15±8.08 stem cells per HPF), illustrating increased stem-like cells in animals that are more prone to neoplasia. DCAMKL1 labeled stem-like cells were equal in number in the male and female groups receiving the control AIN 76A diet alone (females, 25.73 stem-like cells/HPF); males, 24.15 stem-like cells/HPF). However, females showed a greater reduction in the number of DCAMKL1-labeled stem-like cells with celecoxib supplementation than the respective males (16.63±4.23 vs. 21.56±9.06; a reduction of 35.4% in females to 10.7% in males). We conclude that a higher number of stem-like cells in the uninvolved mucosa paralleled tumorigenesis and mirrored greater chemopreventive responsiveness of female MIN mice compared to males.

KW - Celecoxib

KW - Chemoprevention

KW - Doublecortin and calcium/calmodulin- dependent protein kinase-like-1

KW - Gender

KW - Intestine

KW - Stem-like cells

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Association of stem-like cells in gender-specific chemoprevention against intestinal neoplasia in MIN mouse

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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