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1Department of Surgery, University of Ulsan College of Medicine and Asan Medical Center, Seoul, Korea
2Laboratory of Cancer Biology and Genetics, Asan Institute for Life Sciences, Asan Medical Center, Seoul, Korea
3Cancer and Immunogenetics Laboratory, Weatherall Institute of Molecular Medicine, John Radcliffe Hospital, University of Oxford, Oxford, United Kingdom
Copyright © 2021 The Korean Society of Coloproctology
This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0/) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
CONFLICT OF INTEREST
No potential conflict of interest relevant to this article was reported.
Syndrome | Causative gene/clinical manifestation |
Lifetime risk of associate neoplasmsa (%) |
|||||||||
---|---|---|---|---|---|---|---|---|---|---|---|
Colon | Stomach | Small bowel | Pancreas | Breast | Endometrial | Ovary | Urinary | Thyroid | Others | ||
LS | MMR genes (AD): MLH, MSH2, MSH6, PMS2 | 40–70 | 6–13 | 1–4 | 1–4 | 32–45 | 4–12 | 5–21 | |||
Muir-Torreb | MMR genes (65%, AD), MUTYH (35%, AR) | 40–70 | 6–13 | 1–4 | 1–4 | 15 | 4–12 | 5–21 | Skin | ||
Turcotb | MMR genes (AR)/LS, GB | 40–70 | 6–13 | 1–4 | 1–4 | 32–45 | 4–12 | 5–21 | 5–20 | GB/MB | |
APC (AR), FAP, MB | |||||||||||
CMMRD | MMR genes (AD): particularly PMS2, MSH6/café au lait | 32 (colon+stomach+SB) | GB, H | ||||||||
EALS | EPCAM, MSH2 silencing/congenital tufting enteropathy | 40–70 | 6–13 | Moderately increase risk of CRC/lower risk of extracolonic cancer | |||||||
FCCTX | Unidentified genes/site-specific distal CRC with later age onset | Moderately increase risk of CRC/lower risk of extracolonic cancer |
LS, Lynch syndrome; MMR, mismatch repair genes; AD, autosomal dominant; AR, autosomal recessive; GB, glioblastoma; FAP, familial adenomatous polyposis; MB, medulloblastoma; CMMRD, constitutional MMR deficiency; SB, small bowel; H, hematological malignancy; EALS, EPCAM-associated LS; CRC, colorectal cancer; FCCTX, famili-al colorectal cancer type X.
aLifetime syndrome risks mostly based on the American College of Gastroenterology Guideline of Hereditary Gastrointestinal Cancer Syndromes (2015; https://gi.org/guidelines/) and included references.
bPredicted on the basis of LS with additional FAP in Turcot syndrome.
Syndrome | Causative gene | Clinical manifestations |
Lifetime syndrome risk of associate neoplasmsa (%) |
|||||||||
---|---|---|---|---|---|---|---|---|---|---|---|---|
Colon | Stomach | Small bowel | Pancreas | Breast | Endometrial | Ovary | Urinary | Thyroid | Others | |||
FAP | APC (AD) | Benign soft tissue tumor, CHRPE | 90 (69b) | 2–5 | 5–20 | 2–5 | 5–20 | Desmoid, MB | ||||
MAP | MUTYH (AD) | CRC-proximal colon, mucin, LC infiltration | 43–63 | Less common than those in FAP, otherwise similar spectrum to LS | ||||||||
PPAP | POLE, POLD1 (AD) | LS-like phenotype in a minority | 70 | 9.5 | 12 | IR | ||||||
Sessile polyposis | RNF43 (AD) | ≥5, >rectum (≥2, ≥10 mm), ≥20 (≥5, >rectum) | 20 | Undetermined | ||||||||
Peutz-Jeghers | STK11 (AD) | Mucocutaneous pigmented macules | 40 | 5–20 | 2–5 | 5–20 | 50 | 10 | 20 | |||
JP | SMAD4, BMPR1A (AD) | ≥5, extrabowel JP, family history | 20–40 | 5–20 | ||||||||
PHTS | PTEN, PTCH (AD) | Including BRRS, CS, GS, PS; Upper GIc | 9 | 85 | 28 | 34 | 35 | Melanoma | ||||
HMPS | SCG5/GREM1 (AD) | Adenoma, serrated/inflammatory polyp | Undetermined |
FAP, familial adenomatous polyposis; AD, autosomal dominant; CHRPE, congenital hypertrophy of retinal pigment epithelium; MB, medulloblastoma; MAP, MUTYH-associated polyposis; CRC, colorectal cancer; LC, lymphocyte; LS, Lynch syndrome; PPAP, polymerase-proofreading-associated polyposis; IR, increased rate; JP, Juvenile polyposis; PHTS, PTEN hamartoma tumor syndrome; BRRS, Bannayan-Riley-Ruvalcaba syndrome; CS, Cowden syndrome; GS, Gorlin syndrome; PS, Proteus-like syndromes; GI, gastrointestinal; HMPS, hereditary mixed polyposis.
aLifetime syndrome risks mostly based on the American College of Gastroenterology Guideline of Hereditary Gastrointestinal Cancer Syndromes (2015; https://gi.org/guidelines/) and included refer-ences; PPAP based on the National Study of Colorectal Cancer Genetics (2013), UK; PHTS based on the International Cowden Consortium (2012).
bRisk in the parenthesis indicates lifetime risk (%) in attenuated FAP.
cThe most common upper GI lesions are esophageal glycogenic acanthosis (37%), gastric hamartomatous polyps (47%), and duodenal hamartomatous polyps (20%).
Syndrome | Organ | Start age (yr) | Interval (yr) | Procedure | GRADEa |
---|---|---|---|---|---|
LS and LS-spectrumb | Colon | 20–25 | 1–2 | Colonoscopy | High |
EM, cervix, ovary | 30–35 | 1–2 | Biopsy, USG, PS | Moderate | |
Stomach, duodenum | 30–35 | 1–3 | EGD | Moderate | |
Urinary tract | 20–35 | 1 | Urinalysis | Very low | |
Pancreas | 35–40 | 1–3 | MRI, ERCP | Low | |
EALS | Colon | 20–25 | 1–2 | Colonoscopy | High |
Stomach, duodenum | 30–35 | 1–3 | EGD | Moderate | |
FCCTX | Colon | 20–25 | 1–2 | Colonoscopy | Moderate |
FAP | Colon | 12–14 | 1–2 | Colonoscopy | High |
Stomach, duodenum | 25–30 | 1–3 | EGD | Moderate | |
Thyroid | 15–20 | 1–2 | PE and USG | Low | |
Attenuated FAP | Colon | 18–20 | 1–3 | Colonoscopy | High |
Stomach, duodenum | 25–30 | 1–3 | EGD | Moderate | |
MAP | Colon | 18–20 | 1–2 | Colonoscopy | High |
Stomach, duodenum | 25–30 | 1–3 | EGD | Moderate | |
PPAP | Colon | 25–30 | 1–3 | Colonoscopy | Moderate |
Stomach, duodenum | 25–30 | 1–3 | EGD | Low | |
EM, cervix, ovary | 25–30 | 1–2 | Biopsy, USG, PS | Low | |
SPS | Colon | Undetermined | 1–3 | Colonoscopy | Moderate |
PJS | Colon | 10, 18c | 3 | Colonoscopy | High |
Upper GI | 10, 18c | 3 | EGD, enteroscopy | High | |
Pancreas | 30 | 1–3 | MRI, ERCP | Moderate | |
Breast | 25 | 1 | PE, MG, USG | Moderate | |
EM, cervix, ovary | 25 | 1–2 | Biopsy, USG, PS | Low | |
Testis | Birth–teenage | 1 | PE, USG | Low | |
JPS | Colon | 12–15 | 1–3 | Colonoscopy | Moderate |
Stomach, duodenum | 12–15 | 1–3 | EGD | Low | |
PTHS | Colon | 15 | 1–3 | Colonoscopy | High |
Stomach, duodenum | 15 | 1–3 | EGD | Moderate | |
Breast | 25–35 | 1 | PE, MG, USG | Moderate | |
EM, cervix, ovary | 30–35 | 1–2 | Biopsy, USG, PS | Low | |
Thyroid | 15–20 | 1 | PE and USG | Low | |
Kidney (renal cell) | 18 | 1 | Urinalysis, USG | Low | |
Skin (melanoma) | By 18 | 1 | PE | Low | |
HMPS | Colon | Undetermined | 1–3 | Colonoscopy | Low |
LS, Lynch syndrome; EM, endometrium; USG, ultrasonography; PS, Pap smear; EGD, esophagoduodenoscopy; MRI, magnetic resonance imaging; ERCP, endoscopic retrograde cholangiopancreatography; EALS, EPCAM-associated LS; FCCTX, familial colorectal cancer type X; FAP, familial adenomatous polyposis; PE, physical examination; MAP, MUTYH-associated polyposis; PPAP, polymerase-proofreading-associated polyposis; SPS, sessile polyposis syndrome; PJS, Peutz-Jeghers syndrome; GI, gastrointestinal; MG, mammography; JPS, juvenile polyposis syndrome; PTHS, PTEN hamartoma syndrome; HMPS, hereditary mixed polyposis syndrome.
aGRADE (Grading of Recommendations Assessment, Development and Evaluation) system was used to grade the strength of recommendations and the quality of evidence.
bLS-spectrum includes Muir-Torre syndrome, Turcot syndrome, and constitutional mismatch repair deficiency.
cAt age of 8 years, if present every 3 years; if no polyps, repeat at age of 18 years, then every 3 years or earlier on symptom.
Syndrome | Causative gene/clinical manifestation | Lifetime risk of associate neoplasms |
|||||||||
---|---|---|---|---|---|---|---|---|---|---|---|
Colon | Stomach | Small bowel | Pancreas | Breast | Endometrial | Ovary | Urinary | Thyroid | Others | ||
LS | MMR genes (AD): MLH, MSH2, MSH6, PMS2 | 40–70 | 6–13 | 1–4 | 1–4 | 32–45 | 4–12 | 5–21 | |||
Muir-Torre |
MMR genes (65%, AD), MUTYH (35%, AR) | 40–70 | 6–13 | 1–4 | 1–4 | 15 | 4–12 | 5–21 | Skin | ||
Turcot |
MMR genes (AR)/LS, GB | 40–70 | 6–13 | 1–4 | 1–4 | 32–45 | 4–12 | 5–21 | 5–20 | GB/MB | |
APC (AR), FAP, MB | |||||||||||
CMMRD | MMR genes (AD): particularly PMS2, MSH6/café au lait | 32 (colon+stomach+SB) | GB, H | ||||||||
EALS | EPCAM, MSH2 silencing/congenital tufting enteropathy | 40–70 | 6–13 | Moderately increase risk of CRC/lower risk of extracolonic cancer | |||||||
FCCTX | Unidentified genes/site-specific distal CRC with later age onset | Moderately increase risk of CRC/lower risk of extracolonic cancer |
Syndrome | Causative gene | Clinical manifestations | Lifetime syndrome risk of associate neoplasms |
|||||||||
---|---|---|---|---|---|---|---|---|---|---|---|---|
Colon | Stomach | Small bowel | Pancreas | Breast | Endometrial | Ovary | Urinary | Thyroid | Others | |||
FAP | APC (AD) | Benign soft tissue tumor, CHRPE | 90 (69 |
2–5 | 5–20 | 2–5 | 5–20 | Desmoid, MB | ||||
MAP | MUTYH (AD) | CRC-proximal colon, mucin, LC infiltration | 43–63 | Less common than those in FAP, otherwise similar spectrum to LS | ||||||||
PPAP | POLE, POLD1 (AD) | LS-like phenotype in a minority | 70 | 9.5 | 12 | IR | ||||||
Sessile polyposis | RNF43 (AD) | ≥5, >rectum (≥2, ≥10 mm), ≥20 (≥5, >rectum) | 20 | Undetermined | ||||||||
Peutz-Jeghers | STK11 (AD) | Mucocutaneous pigmented macules | 40 | 5–20 | 2–5 | 5–20 | 50 | 10 | 20 | |||
JP | SMAD4, BMPR1A (AD) | ≥5, extrabowel JP, family history | 20–40 | 5–20 | ||||||||
PHTS | PTEN, PTCH (AD) | Including BRRS, CS, GS, PS; Upper GI |
9 | 85 | 28 | 34 | 35 | Melanoma | ||||
HMPS | SCG5/GREM1 (AD) | Adenoma, serrated/inflammatory polyp | Undetermined |
Syndrome | Organ | Start age (yr) | Interval (yr) | Procedure | GRADE |
---|---|---|---|---|---|
LS and LS-spectrum |
Colon | 20–25 | 1–2 | Colonoscopy | High |
EM, cervix, ovary | 30–35 | 1–2 | Biopsy, USG, PS | Moderate | |
Stomach, duodenum | 30–35 | 1–3 | EGD | Moderate | |
Urinary tract | 20–35 | 1 | Urinalysis | Very low | |
Pancreas | 35–40 | 1–3 | MRI, ERCP | Low | |
EALS | Colon | 20–25 | 1–2 | Colonoscopy | High |
Stomach, duodenum | 30–35 | 1–3 | EGD | Moderate | |
FCCTX | Colon | 20–25 | 1–2 | Colonoscopy | Moderate |
FAP | Colon | 12–14 | 1–2 | Colonoscopy | High |
Stomach, duodenum | 25–30 | 1–3 | EGD | Moderate | |
Thyroid | 15–20 | 1–2 | PE and USG | Low | |
Attenuated FAP | Colon | 18–20 | 1–3 | Colonoscopy | High |
Stomach, duodenum | 25–30 | 1–3 | EGD | Moderate | |
MAP | Colon | 18–20 | 1–2 | Colonoscopy | High |
Stomach, duodenum | 25–30 | 1–3 | EGD | Moderate | |
PPAP | Colon | 25–30 | 1–3 | Colonoscopy | Moderate |
Stomach, duodenum | 25–30 | 1–3 | EGD | Low | |
EM, cervix, ovary | 25–30 | 1–2 | Biopsy, USG, PS | Low | |
SPS | Colon | Undetermined | 1–3 | Colonoscopy | Moderate |
PJS | Colon | 10, 18 |
3 | Colonoscopy | High |
Upper GI | 10, 18 |
3 | EGD, enteroscopy | High | |
Pancreas | 30 | 1–3 | MRI, ERCP | Moderate | |
Breast | 25 | 1 | PE, MG, USG | Moderate | |
EM, cervix, ovary | 25 | 1–2 | Biopsy, USG, PS | Low | |
Testis | Birth–teenage | 1 | PE, USG | Low | |
JPS | Colon | 12–15 | 1–3 | Colonoscopy | Moderate |
Stomach, duodenum | 12–15 | 1–3 | EGD | Low | |
PTHS | Colon | 15 | 1–3 | Colonoscopy | High |
Stomach, duodenum | 15 | 1–3 | EGD | Moderate | |
Breast | 25–35 | 1 | PE, MG, USG | Moderate | |
EM, cervix, ovary | 30–35 | 1–2 | Biopsy, USG, PS | Low | |
Thyroid | 15–20 | 1 | PE and USG | Low | |
Kidney (renal cell) | 18 | 1 | Urinalysis, USG | Low | |
Skin (melanoma) | By 18 | 1 | PE | Low | |
HMPS | Colon | Undetermined | 1–3 | Colonoscopy | Low |
LS, Lynch syndrome; MMR, mismatch repair genes; AD, autosomal dominant; AR, autosomal recessive; GB, glioblastoma; FAP, familial adenomatous polyposis; MB, medulloblastoma; CMMRD, constitutional MMR deficiency; SB, small bowel; H, hematological malignancy; EALS, Lifetime syndrome risks mostly based on the American College of Gastroenterology Guideline of Hereditary Gastrointestinal Cancer Syndromes (2015; Predicted on the basis of LS with additional FAP in Turcot syndrome.
FAP, familial adenomatous polyposis; AD, autosomal dominant; CHRPE, congenital hypertrophy of retinal pigment epithelium; MB, medulloblastoma; MAP, Lifetime syndrome risks mostly based on the American College of Gastroenterology Guideline of Hereditary Gastrointestinal Cancer Syndromes (2015; Risk in the parenthesis indicates lifetime risk (%) in attenuated FAP. The most common upper GI lesions are esophageal glycogenic acanthosis (37%), gastric hamartomatous polyps (47%), and duodenal hamartomatous polyps (20%).
LS, Lynch syndrome; EM, endometrium; USG, ultrasonography; PS, Pap smear; EGD, esophagoduodenoscopy; MRI, magnetic resonance imaging; ERCP, endoscopic retrograde cholangiopancreatography; EALS, EPCAM-associated LS; FCCTX, familial colorectal cancer type X; FAP, familial adenomatous polyposis; PE, physical examination; MAP, MUTYH-associated polyposis; PPAP, polymerase-proofreading-associated polyposis; SPS, sessile polyposis syndrome; PJS, Peutz-Jeghers syndrome; GI, gastrointestinal; MG, mammography; JPS, juvenile polyposis syndrome; PTHS, PTEN hamartoma syndrome; HMPS, hereditary mixed polyposis syndrome. GRADE (Grading of Recommendations Assessment, Development and Evaluation) system was used to grade the strength of recommendations and the quality of evidence. LS-spectrum includes Muir-Torre syndrome, Turcot syndrome, and constitutional mismatch repair deficiency. At age of 8 years, if present every 3 years; if no polyps, repeat at age of 18 years, then every 3 years or earlier on symptom.