Colon and Rectal Cancer Survival by Tumor Location and Microsatellite Instability: The Colon Cancer Family Registry

BACKGROUND:Cancers in the proximal colon, distal colon, and rectum are frequently studied together; however, there are biological differences in cancers across these sites, particularly in the prevalence of microsatellite instability. OBJECTIVE:We assessed the differences in survival by colon or rec...

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Published inDiseases of the colon & rectum Vol. 56; no. 8; pp. 937 - 944
Main Authors Phipps, Amanda I., Lindor, Noralane M., Jenkins, Mark A., Baron, John A., Win, Aung Ko, Gallinger, Steven, Gryfe, Robert, Newcomb, Polly A.
Format Journal Article
LanguageEnglish
Published Hagerstown, MDc The American Society of Colon and Rectal Surgeons 01.08.2013
Lippincott Williams & Wilkins
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Online AccessGet full text
ISSN0012-3706
1530-0358
1530-0358
DOI10.1097/DCR.0b013e31828f9a57

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Abstract BACKGROUND:Cancers in the proximal colon, distal colon, and rectum are frequently studied together; however, there are biological differences in cancers across these sites, particularly in the prevalence of microsatellite instability. OBJECTIVE:We assessed the differences in survival by colon or rectal cancer site, considering the contribution of microsatellite instability to such differences. DESIGN:This is a population-based prospective cohort study for cancer survival. SETTINGS:This study was conducted within the Colon Cancer Family Registry, an international consortium. Participants were identified from population-based cancer registries in the United States, Canada, and Australia. PATIENTS:Information on tumor site, microsatellite instability, and survival after diagnosis was available for 3284 men and women diagnosed with incident invasive colon or rectal cancer between 1997 and 2002, with ages at diagnosis ranging from 18 to 74. MAIN OUTCOME MEASURES:Cox regression was used to calculate hazard ratios for the association between all-cause mortality and tumor location, overall and by microsatellite instability status. RESULTS:Distal colon (HR, 0.59; 95% CI, 0.49–0.71) and rectal cancers (HR, 0.68; 95% CI, 0.57–0.81) were associated with lower mortality than proximal colon cancer overall. Compared specifically with patients with proximal colon cancer exhibiting no/low microsatellite instability, patients with distal colon and rectal cancers experienced lower mortality, regardless of microsatellite instability status; patients with proximal colon cancer exhibiting high microsatellite instability had the lowest mortality. LIMITATIONS:Study limitations include the absence of stage at diagnosis and cause-of-death information for all but a subset of study participants. Some patient groups defined jointly by tumor site and microsatellite instability status are subject to small numbers. CONCLUSION:Proximal colon cancer survival differs from survival for distal colon and rectal cancer in a manner apparently dependent on microsatellite instability status. These findings support the premise that proximal colon, distal colon, and rectal cancers are clinicopathologically distinct.
AbstractList BACKGROUND:Cancers in the proximal colon, distal colon, and rectum are frequently studied together; however, there are biological differences in cancers across these sites, particularly in the prevalence of microsatellite instability. OBJECTIVE:We assessed the differences in survival by colon or rectal cancer site, considering the contribution of microsatellite instability to such differences. DESIGN:This is a population-based prospective cohort study for cancer survival. SETTINGS:This study was conducted within the Colon Cancer Family Registry, an international consortium. Participants were identified from population-based cancer registries in the United States, Canada, and Australia. PATIENTS:Information on tumor site, microsatellite instability, and survival after diagnosis was available for 3284 men and women diagnosed with incident invasive colon or rectal cancer between 1997 and 2002, with ages at diagnosis ranging from 18 to 74. MAIN OUTCOME MEASURES:Cox regression was used to calculate hazard ratios for the association between all-cause mortality and tumor location, overall and by microsatellite instability status. RESULTS:Distal colon (HR, 0.59; 95% CI, 0.49–0.71) and rectal cancers (HR, 0.68; 95% CI, 0.57–0.81) were associated with lower mortality than proximal colon cancer overall. Compared specifically with patients with proximal colon cancer exhibiting no/low microsatellite instability, patients with distal colon and rectal cancers experienced lower mortality, regardless of microsatellite instability status; patients with proximal colon cancer exhibiting high microsatellite instability had the lowest mortality. LIMITATIONS:Study limitations include the absence of stage at diagnosis and cause-of-death information for all but a subset of study participants. Some patient groups defined jointly by tumor site and microsatellite instability status are subject to small numbers. CONCLUSION:Proximal colon cancer survival differs from survival for distal colon and rectal cancer in a manner apparently dependent on microsatellite instability status. These findings support the premise that proximal colon, distal colon, and rectal cancers are clinicopathologically distinct.
Cancers in the proximal colon, distal colon, and rectum are frequently studied together; however, there are biological differences in cancers across these sites, particularly in the prevalence of microsatellite instability. We assessed the differences in survival by colon or rectal cancer site, considering the contribution of microsatellite instability to such differences. This is a population-based prospective cohort study for cancer survival. This study was conducted within the Colon Cancer Family Registry, an international consortium. Participants were identified from population-based cancer registries in the United States, Canada, and Australia. Information on tumor site, microsatellite instability, and survival after diagnosis was available for 3284 men and women diagnosed with incident invasive colon or rectal cancer between 1997 and 2002, with ages at diagnosis ranging from 18 to 74. Cox regression was used to calculate hazard ratios for the association between all-cause mortality and tumor location, overall and by microsatellite instability status. Distal colon (HR, 0.59; 95% CI, 0.49-0.71) and rectal cancers (HR, 0.68; 95% CI, 0.57-0.81) were associated with lower mortality than proximal colon cancer overall. Compared specifically with patients with proximal colon cancer exhibiting no/low microsatellite instability, patients with distal colon and rectal cancers experienced lower mortality, regardless of microsatellite instability status; patients with proximal colon cancer exhibiting high microsatellite instability had the lowest mortality. Study limitations include the absence of stage at diagnosis and cause-of-death information for all but a subset of study participants. Some patient groups defined jointly by tumor site and microsatellite instability status are subject to small numbers. Proximal colon cancer survival differs from survival for distal colon and rectal cancer in a manner apparently dependent on microsatellite instability status. These findings support the premise that proximal colon, distal colon, and rectal cancers are clinicopathologically distinct.
Cancers in the proximal colon, distal colon, and rectum are frequently studied together; however, there are biological differences in cancers across these sites, particularly in the prevalence of microsatellite instability.BACKGROUNDCancers in the proximal colon, distal colon, and rectum are frequently studied together; however, there are biological differences in cancers across these sites, particularly in the prevalence of microsatellite instability.We assessed the differences in survival by colon or rectal cancer site, considering the contribution of microsatellite instability to such differences.OBJECTIVEWe assessed the differences in survival by colon or rectal cancer site, considering the contribution of microsatellite instability to such differences.This is a population-based prospective cohort study for cancer survival.DESIGNThis is a population-based prospective cohort study for cancer survival.This study was conducted within the Colon Cancer Family Registry, an international consortium. Participants were identified from population-based cancer registries in the United States, Canada, and Australia.SETTINGSThis study was conducted within the Colon Cancer Family Registry, an international consortium. Participants were identified from population-based cancer registries in the United States, Canada, and Australia.Information on tumor site, microsatellite instability, and survival after diagnosis was available for 3284 men and women diagnosed with incident invasive colon or rectal cancer between 1997 and 2002, with ages at diagnosis ranging from 18 to 74.PATIENTSInformation on tumor site, microsatellite instability, and survival after diagnosis was available for 3284 men and women diagnosed with incident invasive colon or rectal cancer between 1997 and 2002, with ages at diagnosis ranging from 18 to 74.Cox regression was used to calculate hazard ratios for the association between all-cause mortality and tumor location, overall and by microsatellite instability status.MAIN OUTCOME MEASURESCox regression was used to calculate hazard ratios for the association between all-cause mortality and tumor location, overall and by microsatellite instability status.Distal colon (HR, 0.59; 95% CI, 0.49-0.71) and rectal cancers (HR, 0.68; 95% CI, 0.57-0.81) were associated with lower mortality than proximal colon cancer overall. Compared specifically with patients with proximal colon cancer exhibiting no/low microsatellite instability, patients with distal colon and rectal cancers experienced lower mortality, regardless of microsatellite instability status; patients with proximal colon cancer exhibiting high microsatellite instability had the lowest mortality.RESULTSDistal colon (HR, 0.59; 95% CI, 0.49-0.71) and rectal cancers (HR, 0.68; 95% CI, 0.57-0.81) were associated with lower mortality than proximal colon cancer overall. Compared specifically with patients with proximal colon cancer exhibiting no/low microsatellite instability, patients with distal colon and rectal cancers experienced lower mortality, regardless of microsatellite instability status; patients with proximal colon cancer exhibiting high microsatellite instability had the lowest mortality.Study limitations include the absence of stage at diagnosis and cause-of-death information for all but a subset of study participants. Some patient groups defined jointly by tumor site and microsatellite instability status are subject to small numbers.LIMITATIONSStudy limitations include the absence of stage at diagnosis and cause-of-death information for all but a subset of study participants. Some patient groups defined jointly by tumor site and microsatellite instability status are subject to small numbers.Proximal colon cancer survival differs from survival for distal colon and rectal cancer in a manner apparently dependent on microsatellite instability status. These findings support the premise that proximal colon, distal colon, and rectal cancers are clinicopathologically distinct.CONCLUSIONProximal colon cancer survival differs from survival for distal colon and rectal cancer in a manner apparently dependent on microsatellite instability status. These findings support the premise that proximal colon, distal colon, and rectal cancers are clinicopathologically distinct.
Author Lindor, Noralane M.
Phipps, Amanda I.
Gryfe, Robert
Jenkins, Mark A.
Gallinger, Steven
Win, Aung Ko
Newcomb, Polly A.
Baron, John A.
AuthorAffiliation 1 Public Health Sciences Division, Fred Hutchinson Cancer Research Center, Seattle, Washington 2 Department of Epidemiology, University of Washington, Seattle, Washington 3 Department of Medical Genetics, Mayo Clinic, Rochester, Minnesota 4 Centre for Molecular, Environmental, Genetic and Analytic Epidemiology, Melbourne School of Population Health, The University of Melbourne, Parkville, Victoria, Australia 5 Department of Medicine, University of North Carolina, Chapel Hill, North Carolina 6 Cancer Care Ontario, Toronto, Ontario, Canada
AuthorAffiliation_xml – name: 1 Public Health Sciences Division, Fred Hutchinson Cancer Research Center, Seattle, Washington 2 Department of Epidemiology, University of Washington, Seattle, Washington 3 Department of Medical Genetics, Mayo Clinic, Rochester, Minnesota 4 Centre for Molecular, Environmental, Genetic and Analytic Epidemiology, Melbourne School of Population Health, The University of Melbourne, Parkville, Victoria, Australia 5 Department of Medicine, University of North Carolina, Chapel Hill, North Carolina 6 Cancer Care Ontario, Toronto, Ontario, Canada
– name: 1 Cancer Prevention Program, Fred Hutchinson Cancer Research Center, Seattle, WA, USA
– name: 5 Department of Medicine, University of North Carolina, Chapel Hill, NC, USA
– name: 2 Department of Epidemiology, University of Washington, Seattle, WA, USA
– name: 3 Department of Medical Genetics, Mayo Clinic, Rochester, MN, USA
– name: 4 Centre for Molecular, Environmental, Genetic and Analytic Epidemiology, Melbourne School of Population Health, The University of Melbourne, Parkville, Victoria, Australia
– name: 6 Cancer Care Ontario, Toronto, Ontario, Canada
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  givenname: Amanda
  surname: Phipps
  middlename: I.
  fullname: Phipps, Amanda I.
  organization: 1 Public Health Sciences Division, Fred Hutchinson Cancer Research Center, Seattle, Washington 2 Department of Epidemiology, University of Washington, Seattle, Washington 3 Department of Medical Genetics, Mayo Clinic, Rochester, Minnesota 4 Centre for Molecular, Environmental, Genetic and Analytic Epidemiology, Melbourne School of Population Health, The University of Melbourne, Parkville, Victoria, Australia 5 Department of Medicine, University of North Carolina, Chapel Hill, North Carolina 6 Cancer Care Ontario, Toronto, Ontario, Canada
– sequence: 2
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  surname: Lindor
  middlename: M.
  fullname: Lindor, Noralane M.
– sequence: 3
  givenname: Mark
  surname: Jenkins
  middlename: A.
  fullname: Jenkins, Mark A.
– sequence: 4
  givenname: John
  surname: Baron
  middlename: A.
  fullname: Baron, John A.
– sequence: 5
  givenname: Aung
  surname: Win
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  fullname: Win, Aung Ko
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  surname: Gryfe
  fullname: Gryfe, Robert
– sequence: 8
  givenname: Polly
  surname: Newcomb
  middlename: A.
  fullname: Newcomb, Polly A.
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Issue 8
Keywords Rectal disease
Prognosis
Rectal cancer
Family study
Colorectal cancer
Malignant tumor
Rectum cancer
Microsatellite instability
Rectal tumor
Survival
Colonic disease
Colon cancer
Microsatellite DNA
Gastroenterology
Digestive diseases
Intestinal disease
Instability
Anorectal disease
Cancer
Language English
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PublicationDate 2013-August
PublicationDateYYYYMMDD 2013-08-01
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  year: 2013
  text: 2013-August
PublicationDecade 2010
PublicationPlace Hagerstown, MDc
PublicationPlace_xml – name: Hagerstown, MDc
– name: United States
PublicationTitle Diseases of the colon & rectum
PublicationTitleAlternate Dis Colon Rectum
PublicationYear 2013
Publisher The American Society of Colon and Rectal Surgeons
Lippincott Williams & Wilkins
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Snippet BACKGROUND:Cancers in the proximal colon, distal colon, and rectum are frequently studied together; however, there are biological differences in cancers across...
Cancers in the proximal colon, distal colon, and rectum are frequently studied together; however, there are biological differences in cancers across these...
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SubjectTerms Adolescent
Adult
Aged
Australia - epidemiology
Biological and medical sciences
Biomarkers, Tumor - genetics
Canada - epidemiology
Colon - pathology
Colonic Neoplasms - genetics
Colonic Neoplasms - mortality
CpG Islands
DNA, Neoplasm - genetics
Female
Follow-Up Studies
Gastroenterology. Liver. Pancreas. Abdomen
Humans
Male
Medical sciences
Microsatellite Instability
Middle Aged
Multiple tumors. Solid tumors. Tumors in childhood (general aspects)
Prospective Studies
Proto-Oncogene Proteins B-raf - genetics
Rectal Neoplasms - genetics
Rectal Neoplasms - mortality
Rectum - pathology
Registries
Stomach. Duodenum. Small intestine. Colon. Rectum. Anus
Survival Rate - trends
Time Factors
Tumors
United States - epidemiology
Young Adult
Title Colon and Rectal Cancer Survival by Tumor Location and Microsatellite Instability: The Colon Cancer Family Registry
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https://www.ncbi.nlm.nih.gov/pubmed/23838861
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