Villous adenoma: Difference between revisions
Jump to navigation
Jump to search
| Line 7: | Line 7: | ||
==Overview== | ==Overview== | ||
'''Villous adenoma''' (also known as adenomatous polyp) is a type of [[polyp (medicine)|polyp]] that grows in the [[gastrointestinal tract]]; it occurs most commonly in the [[colon]]. Villous adenoma may result in [[malignant]] | '''Villous adenoma''' (also known as adenomatous polyp) is a type of [[polyp (medicine)|polyp]] that grows in the [[gastrointestinal tract]]; it occurs most commonly in the [[colon]]. Villous adenoma may result in [[malignant]]<nowiki/>transformation. Villous adenoma was first discovered by Helwig in 1946. Villous adenoma may be classified into flat, sessile, pedunculated and depressed subtypes. Villous adenoma arises from [[Epithelium|epithelial]] tissue, which is normally part of the lining of the colon. Genes associated with the development of villous adenoma include [[APC]], [[TP53]], [[KRAS|K-ras]], STK11 and SMAD4. The [[prevalence]] of villous adenoma is approximately 3.5 per 100,000 individuals worldwide. The most potent risk factors in the development of villous adenoma include familial syndromes such as [[Turcot syndrome|Turcot syndrome]], [[Juvenile polyposis syndrome|juvenile polyposis syndrome]], and [[Cowden disease]]. Surgical removal is the mainstay of therapy for villous adenoma. Exploratory [[colonoscopy]] and [[Cauterization|cautery]] snare is the most common approach to the diagnosis and treatment of villous adenoma. Effective measures for the primary prevention of villous adenoma include periodic screening of patients with family history of [[familial adenomatous polyposis]]. Secondary prevention strategies include annual [[occult blood test]] and colonoscopy. | ||
==Historical Perspective== | ==Historical Perspective== | ||
| Line 13: | Line 13: | ||
==Classification== | ==Classification== | ||
[[Colon polyps|Colon polyp]]<nowiki/>s are classified into 3 subtypes according to their histological appearance:<ref name="pmid19764676">{{cite journal |vauthors=Osifo OD, Akhiwu W, Efobi CA |title=Small intestinal tubulovillous adenoma--case report and literature review |journal=Niger J Clin Pract |volume=12 |issue=2 |pages=205–7 |year=2009 |pmid=19764676 |doi= |url=}}</ref> | |||
*Tubular | *[[Tubular]] | ||
*Tubulovillous | *Tubulovillous | ||
*Villous | *[[Villous carcinoma|Villous]] | ||
Villous adenoma | Villous adenoma is classified into 4 types according to the gross appearance: | ||
* Flat | * Flat | ||
* Sessile | * Sessile | ||
* Pedunculated | * Pedunculated | ||
* Depressed | * Depressed | ||
Villous adenoma is classified into 2 types according to dysplasia: | Villous adenoma is classified into 2 types according to [[dysplasia]]: | ||
* Low grade dysplasia | * Low grade dysplasia | ||
* High grade dysplasia | * High grade dysplasia | ||
| Line 28: | Line 28: | ||
==Pathophysiology== | ==Pathophysiology== | ||
===Pathogenesis=== | ===Pathogenesis=== | ||
* Villous adenoma is a type of | * Villous adenoma is a type of colon poylp. | ||
* The pathogenesis of villous adenoma is characterized by overgrowth of [[epithelial]] tissue with [[glandular]] characteristics.<ref name="pmid19764676">{{cite journal |vauthors=Osifo OD, Akhiwu W, Efobi CA |title=Small intestinal tubulovillous adenoma--case report and literature review |journal=Niger J Clin Pract |volume=12 |issue=2 |pages=205–7 |year=2009 |pmid=19764676 |doi= |url=}}</ref><ref name="pmid29262150">{{cite journal| author=| title=StatPearls | journal= | year= 2018 | volume= | issue= | pages= | pmid=29262150 | doi= | pmc= | url= }} </ref> | * The pathogenesis of villous adenoma is characterized by overgrowth of [[epithelial]] tissue with [[glandular]] characteristics.<ref name="pmid19764676">{{cite journal |vauthors=Osifo OD, Akhiwu W, Efobi CA |title=Small intestinal tubulovillous adenoma--case report and literature review |journal=Niger J Clin Pract |volume=12 |issue=2 |pages=205–7 |year=2009 |pmid=19764676 |doi= |url=}}</ref><ref name="pmid29262150">{{cite journal| author=| title=StatPearls | journal= | year= 2018 | volume= | issue= | pages= | pmid=29262150 | doi= | pmc= | url= }} </ref> | ||
* Dysplastic changes are present in the adenomas. | * [[Dysplasia|Dysplastic]] changes are present in the adenomas. | ||
* Multiple genetic mutations result in the transition from normal mucosa to adenoma to severe dysplasia and finally to carcinoma | * Multiple genetic [[Mutation|mutations]] result in the transition from normal [[Mucous membrane|mucosa]] to adenoma to severe dysplasia and finally to carcinoma | ||
* Low grade or high-grade dysplasia, which indicates the level of maturation of the epithelium determine the progression of the adenoma. | * Low grade or high-grade dysplasia, which indicates the level of maturation of the epithelium determine the progression of the adenoma. | ||
* Features of low grade dysplasia are: | * Features of low grade dysplasia are: | ||
** The cytological features include crowded, pseudo-stratification to early stratification of spindled or elongated nuclei which occupy the basal half of the cytoplasm.<ref name="pmid12725874">{{cite journal| author=Costantini M, Sciallero S, Giannini A, Gatteschi B, Rinaldi P, Lanzanova G et al.| title=Interobserver agreement in the histologic diagnosis of colorectal polyps. the experience of the multicenter adenoma colorectal study (SMAC). | journal=J Clin Epidemiol | year= 2003 | volume= 56 | issue= 3 | pages= 209-14 | pmid=12725874 | doi= | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=12725874 }} </ref> | ** The cytological features include crowded, pseudo-stratification to early stratification of spindled or elongated [[Cell nucleus|nuclei]] which occupy the basal half of the [[cytoplasm]].<ref name="pmid12725874">{{cite journal| author=Costantini M, Sciallero S, Giannini A, Gatteschi B, Rinaldi P, Lanzanova G et al.| title=Interobserver agreement in the histologic diagnosis of colorectal polyps. the experience of the multicenter adenoma colorectal study (SMAC). | journal=J Clin Epidemiol | year= 2003 | volume= 56 | issue= 3 | pages= 209-14 | pmid=12725874 | doi= | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=12725874 }} </ref> | ||
** Pleomorphism and atypical mitoses are absent. | ** [[Pleomorphism]] and atypical [[Mitosis|mitoses]] are absent. | ||
** The crypts maintain a resemblance to normal colon, without significant crowding, cribriform, or complex forms.The lesions are confined to the epithelial layer of crypts and lack invasion through the basement membrane into the lamina propria. | ** The crypts maintain a resemblance to normal colon, without significant crowding, cribriform, or complex forms.The lesions are confined to the epithelial layer of crypts and lack invasion through the [[basement membrane]] into the [[lamina propria]]. | ||
** As there are no lymphatic vessels in the lamina propria, lesions with low grade dysplasia are not associated with metastasis. | ** As there are no [[Lymphatic system|lymphatic]] vessels in the lamina propria, lesions with low grade dysplasia are not associated with metastasis. | ||
* Features of high grade dysplasia are: | * Features of high grade dysplasia are: | ||
** The cytological features include increased nucleus to cytoplasm ratio, more significant loss of polarity and nuclei with increasingly prominent nucleoli. | ** The cytological features include increased nucleus to cytoplasm ratio, more significant loss of polarity and nuclei with increasingly prominent [[nucleoli]]. | ||
** Significant pleomorphism, rounded nuclei, atypical mitoses, and significant loss of polarity. | ** Significant [[pleomorphism]], rounded nuclei, atypical mitoses, and significant loss of polarity. | ||
** The crypts are cribriform and crowded with back-to-back glandular tissue <ref name="pmid30348703">{{cite journal| author=Rubio CA| title=Preliminary Report: Multiple Clusters of Proliferating Cells in Non-dysplastic Corrupted Colonic Crypts Underneath Conventional Adenomas. | journal=In Vivo | year= 2018 | volume= 32 | issue= 6 | pages= 1473-1475 | pmid=30348703 | doi=10.21873/invivo.11401 | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=30348703 }} </ref>. | ** The crypts are cribriform and crowded with back-to-back [[glandular]] tissue <ref name="pmid30348703">{{cite journal| author=Rubio CA| title=Preliminary Report: Multiple Clusters of Proliferating Cells in Non-dysplastic Corrupted Colonic Crypts Underneath Conventional Adenomas. | journal=In Vivo | year= 2018 | volume= 32 | issue= 6 | pages= 1473-1475 | pmid=30348703 | doi=10.21873/invivo.11401 | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=30348703 }} </ref>. | ||
** These adenomas have a significant risk of metasstasis as the lesions can invade into the lamina propria through basement membrane destruction. | ** These adenomas have a significant risk of metasstasis as the lesions can invade into the lamina propria through basement membrane destruction. | ||
* Villous adenoma can lead to adenocarcinoma of the colon. | * Villous adenoma can lead to [[adenocarcinoma]] of the colon. | ||
* The progression of adenoma-to-carcinoma is dependent on the activation of oncogenes and inactivation of tumor suppresor genes<ref name="pmid15386327">{{cite journal| author=Komuta K, Batts K, Jessurun J, Snover D, Garcia-Aguilar J, Rothenberger D et al.| title=Interobserver variability in the pathological assessment of malignant colorectal polyps. | journal=Br J Surg | year= 2004 | volume= 91 | issue= 11 | pages= 1479-84 | pmid=15386327 | doi=10.1002/bjs.4588 | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=15386327 }} </ref>. | * The progression of adenoma-to-carcinoma is dependent on the activation of [[Oncogene|oncogenes]] and inactivation of [[Tumor suppressor gene|tumor suppresor genes]]<ref name="pmid15386327">{{cite journal| author=Komuta K, Batts K, Jessurun J, Snover D, Garcia-Aguilar J, Rothenberger D et al.| title=Interobserver variability in the pathological assessment of malignant colorectal polyps. | journal=Br J Surg | year= 2004 | volume= 91 | issue= 11 | pages= 1479-84 | pmid=15386327 | doi=10.1002/bjs.4588 | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=15386327 }} </ref>. | ||
* Multiple genetic mutations result in the transition from normal mucosa to adenoma to severe dysplasia and finally to carcinoma. | * Multiple genetic mutations result in the transition from normal mucosa to adenoma to severe dysplasia and finally to carcinoma. | ||
* The genes involved in adenoma formation are: | * The genes involved in adenoma formation are: | ||
** K-ras oncogene | ** K-ras oncogene | ||
** Tumor suppresor p53 gene | ** Tumor suppresor p53 gene | ||
** APC gene on 5 chromosome associated with familial automatosis polyposis syndrome and Gardner | ** [[APC]] gene on 5 chromosome associated with [[FAP|familial automatosis polyposis]] syndrome and [[Gardner's syndrome|Gardner syndrome]] | ||
** [[STK11]] (LBK1) gene, located on [[chromosome]] 19 associated with Peutz-Jeghers syndrome. | ** [[STK11]] (LBK1) gene, located on [[chromosome]] 19 associated with [[Peutz-Jeghers syndrome]]. | ||
** SMAD4 on chromosome 8 associated with juvenile polyposis syndrome. | ** SMAD4 on chromosome 8 associated with [[juvenile polyposis syndrome]]. | ||
* Villous adenomas may cause secretory diarrhea characterized by hypokalemia, chloride-rich stool, and metabolic alkalosis. Increased numbers of goblet cells and increased prostaglandin E2 are responsible for the diarrhea. | * Villous adenomas may cause secretory [[diarrhea]] characterized by [[hypokalemia]], chloride-rich stool, and [[metabolic alkalosis]]. Increased numbers of [[Goblet cell|goblet cells]] and increased [[Prostaglandin E2 receptor|prostaglandin E2]] are responsible for the diarrhea. | ||
[[Image:Colon_adenoma_(1).jpg|thumb|left|[[Colon (anatomy)|Colon]] [[adenoma]] By No machine-readable author provided. KGH assumed (based on copyright claims). - No machine-readable source provided. Own work assumed (based on copyright claims)., CC BY-SA 3.0, https://commons.wikimedia.org/w/index.php?curid=444694]] | [[Image:Colon_adenoma_(1).jpg|thumb|left|[[Colon (anatomy)|Colon]] [[adenoma]] By No machine-readable author provided. KGH assumed (based on copyright claims). - No machine-readable source provided. Own work assumed (based on copyright claims)., CC BY-SA 3.0, https://commons.wikimedia.org/w/index.php?curid=444694]] | ||
<br style="clear:left" /> | <br style="clear:left" /> | ||
| Line 79: | Line 79: | ||
=== Region === | === Region === | ||
* Villous adenomas | * Villous adenomas is common worldwide and has no regional predilection. | ||
==Risk Factors== | ==Risk Factors== | ||
| Line 86: | Line 86: | ||
* African American race | * African American race | ||
* Male sex | * Male sex | ||
* Inflammatory bowel disease | * [[Inflammatory bowel disease]] | ||
* [[Alcoholism|Alcohol abuse]] | * [[Alcoholism|Alcohol abuse]] | ||
* [[Obesity]] | * [[Obesity]] | ||
| Line 106: | Line 106: | ||
===Natural History=== | ===Natural History=== | ||
* The majority of patients with villous adenoma remain asymptomatic for years. | * The majority of patients with villous adenoma remain asymptomatic for years. | ||
* They are usually found accidentally on routine colonoscopic surveillance. | * They are usually found accidentally on routine [[Colonoscopy|colonoscopic]] surveillance. | ||
* Early clinical features may include [[flatulence]], [[bloating]], and [[abdominal pain]]. | * Early clinical features may include [[flatulence]], [[bloating]], and [[abdominal pain]]. | ||
* If left untreated, patients with villous adenoma may progress to develop [[colorectal cancer]].<ref name="pmid19764676">{{cite journal |vauthors=Osifo OD, Akhiwu W, Efobi CA |title=Small intestinal tubulovillous adenoma--case report and literature review |journal=Niger J Clin Pract |volume=12 |issue=2 |pages=205–7 |year=2009 |pmid=19764676 |doi= |url=}}</ref> | * If left untreated, patients with villous adenoma may progress to develop [[colorectal cancer]].<ref name="pmid19764676">{{cite journal |vauthors=Osifo OD, Akhiwu W, Efobi CA |title=Small intestinal tubulovillous adenoma--case report and literature review |journal=Niger J Clin Pract |volume=12 |issue=2 |pages=205–7 |year=2009 |pmid=19764676 |doi= |url=}}</ref> | ||
* The patients may have a previous history of | * The patients may have a previous history of [[colon polyps]]. | ||
* Family history of colon cancer or colon polyps. | * Family history of [[Colorectal cancer|colon cancer]] or colon polyps. | ||
* History of smoking. | * History of smoking. | ||
| Line 116: | Line 116: | ||
Common complications of villous adenoma include: | Common complications of villous adenoma include: | ||
*[[Bleeding|Gatsrointestinal Bleeding]] | *[[Bleeding|Gatsrointestinal Bleeding]] | ||
*Intestinal obstruction | *[[Bowel obstruction|Intestinal obstruction]] | ||
*Progression to [[colorectal cancer]]. | |||
*Progression to colorectal cancer. | |||
===Prognosis=== | ===Prognosis=== | ||
| Line 128: | Line 127: | ||
=== Diagnostic study of choice === | === Diagnostic study of choice === | ||
* Biopsy of the lesion is the diagnostic study of choice. | * [[Biopsy]] of the lesion is the diagnostic study of choice. | ||
* Villous adenoma is detected on colonoscopy or sigmoidoscopy. | * Villous adenoma is detected on colonoscopy or sigmoidoscopy. | ||
| Line 138: | Line 137: | ||
*[[Diarrhea]] | *[[Diarrhea]] | ||
*[[Cramping]] | *[[Cramping]] | ||
*Blood in stools | *[[Gastrointestinal bleeding|Blood in stools]] | ||
*Weight loss | *[[Weight loss]] | ||
*Change in bowel habits | *Change in bowel habits | ||
*Fatigue | *[[Fatigue]] | ||
=== Physical Examination === | === Physical Examination === | ||
Patients with villous adenoma usually appear well but may have the following signs on exmaination. | Patients with villous adenoma usually appear well but may have the following signs on exmaination. | ||
*Pallor due to occult bleeding | *[[Pallor]] due to [[Occult blood|occult]] bleeding | ||
*Abdominal tenderness | *Abdominal tenderness | ||
*Bright red blood on digital rectal examination | *Bright red blood on digital rectal examination | ||
*Rectal mass on digital rectal examination | *[[Rectal masses|Rectal mass]] on digital rectal examination | ||
=== Laboratory Findings === | === Laboratory Findings === | ||
Laboratory findings associated with villous adenoma are: | Laboratory findings associated with villous adenoma are: | ||
* Positive | * Positive [[fecal occult blood test]] | ||
* H[[hypokalemia|ypokalemia]].<ref name="wiki">Villous adenoma. Wikipedia. https://en.wikipedia.org/wiki/Villous_adenoma Accessed on May 3, 2016 </ref> | * H[[hypokalemia|ypokalemia]].<ref name="wiki">Villous adenoma. Wikipedia. https://en.wikipedia.org/wiki/Villous_adenoma Accessed on May 3, 2016 </ref> | ||
* Anemia | * [[Anemia]] | ||
===Other diagnostic studies=== | ===Other diagnostic studies=== | ||
On [[colonoscopy]] and sigmoidoscopy, villous adenoma is visualised as a polyp. | On [[colonoscopy]] and [[sigmoidoscopy]], villous adenoma is visualised as a [[polyp]]. | ||
Alternative imaging studies include: | Alternative imaging studies include: | ||
| Line 167: | Line 166: | ||
* There is no medical therapy for villous adenoma. | * There is no medical therapy for villous adenoma. | ||
* Surgical removal of the adenoma is the mainstay of treatment. | * Surgical removal of the adenoma is the mainstay of treatment. | ||
* However, aspirin 75mg PO per day is recommended to prevent recurrence of the adenoma and progression to colorectal cancer. | * However, [[aspirin]] 75mg PO per day is recommended to prevent recurrence of the adenoma and progression to colorectal cancer. | ||
=== Surgery === | === Surgery === | ||
* Surgical removal is the mainstay of therapy for villous adenoma. | * Surgical removal is the mainstay of therapy for villous adenoma. | ||
* The removal of adenoma is known as polypectomy and is done through colonoscopy. | * The removal of adenoma is known as [[polypectomy]] and is done through colonoscopy by endoscopic forceps snare. | ||
* The removed adenoma is sent for biopsy. | * The removed adenoma is sent for biopsy. | ||
* | * | ||
Revision as of 04:29, 7 February 2019
|
WikiDoc Resources for Villous adenoma |
|
Articles |
|---|
|
Most recent articles on Villous adenoma Most cited articles on Villous adenoma |
|
Media |
|
Powerpoint slides on Villous adenoma |
|
Evidence Based Medicine |
|
Clinical Trials |
|
Ongoing Trials on Villous adenoma at Clinical Trials.gov Trial results on Villous adenoma Clinical Trials on Villous adenoma at Google
|
|
Guidelines / Policies / Govt |
|
US National Guidelines Clearinghouse on Villous adenoma NICE Guidance on Villous adenoma
|
|
Books |
|
News |
|
Commentary |
|
Definitions |
|
Patient Resources / Community |
|
Patient resources on Villous adenoma Discussion groups on Villous adenoma Patient Handouts on Villous adenoma Directions to Hospitals Treating Villous adenoma Risk calculators and risk factors for Villous adenoma
|
|
Healthcare Provider Resources |
|
Causes & Risk Factors for Villous adenoma |
|
Continuing Medical Education (CME) |
|
International |
|
|
|
Business |
|
Experimental / Informatics |
Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Maria Fernanda Villarreal, M.D. [2]
Synonyms and keywords: Adenomatous polyps; VA; TVA
Overview
Villous adenoma (also known as adenomatous polyp) is a type of polyp that grows in the gastrointestinal tract; it occurs most commonly in the colon. Villous adenoma may result in malignanttransformation. Villous adenoma was first discovered by Helwig in 1946. Villous adenoma may be classified into flat, sessile, pedunculated and depressed subtypes. Villous adenoma arises from epithelial tissue, which is normally part of the lining of the colon. Genes associated with the development of villous adenoma include APC, TP53, K-ras, STK11 and SMAD4. The prevalence of villous adenoma is approximately 3.5 per 100,000 individuals worldwide. The most potent risk factors in the development of villous adenoma include familial syndromes such as Turcot syndrome, juvenile polyposis syndrome, and Cowden disease. Surgical removal is the mainstay of therapy for villous adenoma. Exploratory colonoscopy and cautery snare is the most common approach to the diagnosis and treatment of villous adenoma. Effective measures for the primary prevention of villous adenoma include periodic screening of patients with family history of familial adenomatous polyposis. Secondary prevention strategies include annual occult blood test and colonoscopy.
Historical Perspective
Villous adenoma was first discovered by Helwig in 1946.[1]
Classification
Colon polyps are classified into 3 subtypes according to their histological appearance:[2]
Villous adenoma is classified into 4 types according to the gross appearance:
- Flat
- Sessile
- Pedunculated
- Depressed
Villous adenoma is classified into 2 types according to dysplasia:
- Low grade dysplasia
- High grade dysplasia
Pathophysiology
Pathogenesis
- Villous adenoma is a type of colon poylp.
- The pathogenesis of villous adenoma is characterized by overgrowth of epithelial tissue with glandular characteristics.[2][3]
- Dysplastic changes are present in the adenomas.
- Multiple genetic mutations result in the transition from normal mucosa to adenoma to severe dysplasia and finally to carcinoma
- Low grade or high-grade dysplasia, which indicates the level of maturation of the epithelium determine the progression of the adenoma.
- Features of low grade dysplasia are:
- The cytological features include crowded, pseudo-stratification to early stratification of spindled or elongated nuclei which occupy the basal half of the cytoplasm.[4]
- Pleomorphism and atypical mitoses are absent.
- The crypts maintain a resemblance to normal colon, without significant crowding, cribriform, or complex forms.The lesions are confined to the epithelial layer of crypts and lack invasion through the basement membrane into the lamina propria.
- As there are no lymphatic vessels in the lamina propria, lesions with low grade dysplasia are not associated with metastasis.
- Features of high grade dysplasia are:
- The cytological features include increased nucleus to cytoplasm ratio, more significant loss of polarity and nuclei with increasingly prominent nucleoli.
- Significant pleomorphism, rounded nuclei, atypical mitoses, and significant loss of polarity.
- The crypts are cribriform and crowded with back-to-back glandular tissue [5].
- These adenomas have a significant risk of metasstasis as the lesions can invade into the lamina propria through basement membrane destruction.
- Villous adenoma can lead to adenocarcinoma of the colon.
- The progression of adenoma-to-carcinoma is dependent on the activation of oncogenes and inactivation of tumor suppresor genes[6].
- Multiple genetic mutations result in the transition from normal mucosa to adenoma to severe dysplasia and finally to carcinoma.
- The genes involved in adenoma formation are:
- K-ras oncogene
- Tumor suppresor p53 gene
- APC gene on 5 chromosome associated with familial automatosis polyposis syndrome and Gardner syndrome
- STK11 (LBK1) gene, located on chromosome 19 associated with Peutz-Jeghers syndrome.
- SMAD4 on chromosome 8 associated with juvenile polyposis syndrome.
- Villous adenomas may cause secretory diarrhea characterized by hypokalemia, chloride-rich stool, and metabolic alkalosis. Increased numbers of goblet cells and increased prostaglandin E2 are responsible for the diarrhea.
.jpg)
Causes
The cause of villous adneoma is not yet identified.
Differentiating Villous Adenoma from Other Diseases
Villous adenoma must be differentiated from other diseases that cause abnormal growth of tissue projecting from a mucous membrane such as:
- Colorectal cancer
- Inflammatory fibroid polyp
Epidemiology and Demographics
Prevalence
- The prevalence of villous adenoma is approximately 3.5 per 100,000 individuals worldwide.
Age
- Patients of all age groups may develop villous adenoma but the risk increases with age.
Gender
- Males are more commonly affected with villous adenoma than females.
Race
- African Americans are more prone to develop villous adneoma.
Region
- Villous adenomas is common worldwide and has no regional predilection.
Risk Factors
Common risk factors in the development of villous adenoma include[7]:
- Age more than 50 years.
- African American race
- Male sex
- Inflammatory bowel disease
- Alcohol abuse
- Obesity
- Lack of exercise
- Diet high in red meats and processed meats
- Low fiber intake
- Low calcium intake
- Low folate intake
- Type 2 diabetes mellitus
- Familial adenomatous polyposis
- Peutz–Jeghers syndrome
- Turcot syndrome
- Juvenile polyposis syndrome
- Cowden disease
- Bannayan–Riley–Ruvalcaba syndrome (Bannayan-Zonana syndrome)
- Gardner's syndrome
Natural History, Complications and Prognosis
Natural History
- The majority of patients with villous adenoma remain asymptomatic for years.
- They are usually found accidentally on routine colonoscopic surveillance.
- Early clinical features may include flatulence, bloating, and abdominal pain.
- If left untreated, patients with villous adenoma may progress to develop colorectal cancer.[2]
- The patients may have a previous history of colon polyps.
- Family history of colon cancer or colon polyps.
- History of smoking.
Complications
Common complications of villous adenoma include:
- Gatsrointestinal Bleeding
- Intestinal obstruction
- Progression to colorectal cancer.
Prognosis
- The prognosis of villous adenoma is generally good and the 5-year mortality is approximately 89%.
- Prognosis becomes poor with malignant transformation of the lesion.
- Multiple villous adenomas may suggest genetic disorders and prognosis is poor in these cases.
Diagnosis
Diagnostic study of choice
- Biopsy of the lesion is the diagnostic study of choice.
- Villous adenoma is detected on colonoscopy or sigmoidoscopy.
Symptoms
Villous adenoma is commonly asymptomatic but sometimes patients may present with the following symptoms:
- Flatulence
- Abdominal pain
- Constipation
- Diarrhea
- Cramping
- Blood in stools
- Weight loss
- Change in bowel habits
- Fatigue
Physical Examination
Patients with villous adenoma usually appear well but may have the following signs on exmaination.
- Pallor due to occult bleeding
- Abdominal tenderness
- Bright red blood on digital rectal examination
- Rectal mass on digital rectal examination
Laboratory Findings
Laboratory findings associated with villous adenoma are:
- Positive fecal occult blood test
- Hypokalemia.[8]
- Anemia
Other diagnostic studies
On colonoscopy and sigmoidoscopy, villous adenoma is visualised as a polyp.
Alternative imaging studies include:
- CT colonography
- Video capsule endoscopy
Treatment
Medical Therapy
- There is no medical therapy for villous adenoma.
- Surgical removal of the adenoma is the mainstay of treatment.
- However, aspirin 75mg PO per day is recommended to prevent recurrence of the adenoma and progression to colorectal cancer.
Surgery
- Surgical removal is the mainstay of therapy for villous adenoma.
- The removal of adenoma is known as polypectomy and is done through colonoscopy by endoscopic forceps snare.
- The removed adenoma is sent for biopsy.
{{#ev:youtube|ClgRkyhaJZw}}
Prevention
Primary Prevention
Effective measures for the primary prevention of villous adenoma include:
- Periodic screening for polyps in patients with family history of :
- Exercise
- Smoking cessation
- Avoid alcohol
- High fiber diet
Secondary Prevention
- Annual occult blood test
- Colonoscopy every ten years for patients above the age of 50 with no family history of colon cancer or no history of colon polyps.
- Colonoscopy at the age of 40 or 10 years before the age of cancer diagnosis in a relative with colon cancer and repeat every 3-5 years.
- Colonoscopy after polypectomy:
- Every 5 years if 1-2 adenomas present or size <1 cm.
- Every 3 years if 3-10 adenomas present or when size of adenoma is 1-2 cm.
- Every 1-2 years if >10 adenomas present or if size is >2cm.
- Every 2-6 months if signs of adenocarcinoma present.
References
- ↑ Helwig E.B. Adenoma of the large bowel in children. . American Journal of Diseases in Children. 1946;72:289–95
- ↑ 2.0 2.1 2.2 Osifo OD, Akhiwu W, Efobi CA (2009). "Small intestinal tubulovillous adenoma--case report and literature review". Niger J Clin Pract. 12 (2): 205–7. PMID 19764676.
- ↑ "StatPearls". 2018. PMID 29262150.
- ↑ Costantini M, Sciallero S, Giannini A, Gatteschi B, Rinaldi P, Lanzanova G; et al. (2003). "Interobserver agreement in the histologic diagnosis of colorectal polyps. the experience of the multicenter adenoma colorectal study (SMAC)". J Clin Epidemiol. 56 (3): 209–14. PMID 12725874.
- ↑ Rubio CA (2018). "Preliminary Report: Multiple Clusters of Proliferating Cells in Non-dysplastic Corrupted Colonic Crypts Underneath Conventional Adenomas". In Vivo. 32 (6): 1473–1475. doi:10.21873/invivo.11401. PMID 30348703.
- ↑ Komuta K, Batts K, Jessurun J, Snover D, Garcia-Aguilar J, Rothenberger D; et al. (2004). "Interobserver variability in the pathological assessment of malignant colorectal polyps". Br J Surg. 91 (11): 1479–84. doi:10.1002/bjs.4588. PMID 15386327.
- ↑ Jin Y, Yao L, Zhou P, Jin S, Wang X, Tang X; et al. (2018). "[Risk analysis of the canceration of colorectal large polyps]". Zhonghua Wei Chang Wai Ke Za Zhi. 21 (10): 1161–1166. PMID 30370516.
- ↑ Villous adenoma. Wikipedia. https://en.wikipedia.org/wiki/Villous_adenoma Accessed on May 3, 2016