Young-onset colorectal cancer in patients with no known genetic predisposition - Can we increase early recognition and improve outcome?

被引:157
作者
Dozois, Eric J. [1 ]
Boardman, Lisa A. [1 ]
Suwanthanma, Weerapat [1 ]
Limburg, Paul J. [1 ]
Cima, Robert R. [1 ]
Bakken, Julie L. [1 ]
Vierkant, Robert A. [1 ]
Aakre, Jeremiah A. [1 ]
Larson, David W. [1 ]
机构
[1] Mayo Clin, Div Colon & Rectal Surg, Rochester, MN 55905 USA
关键词
D O I
10.1097/MD.0b013e3181881354
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Early recognition of colorectal cancer (CRC) in Young patients without known genetic predisposition is a challenge, and clinicopathologic features at time of presentation are not well described. We conducted the current study to review these features in a large Population of patients with young-onset CRC (initial diagnosis at age <= 50 yr without established risk factors). We reviewed the records of all patients aged 50 years or younger diagnosed with a primary CRC at our institution between 1976 and 2002. Patients with inflammatory bowel disease, polyposis syndromes, or a known genetic predisposition for CRC were excluded. Data regarding clinical and pathologic features at time of initial presentation were abstracted by trained personnel. We identified 1025 patients, 585 male. Mean age at presentation was 42.4 years (standard deviation 6.4). Eight hundred eighty-six (86%) patients were symptomatic at time of diagnosis. Clinical features in symptomatic patients included rectal bleeding (51%), change in bowel habits (18%), abdominal pain (32%), weight loss (13%), nausea/vomiting (7%), melena (2%), and other (26%). Evaluation of asymptomatic patients was pursued with findings of anemia (14%). positive fecal Occult blood test (7%), abdominal mass (2%), mass on digital rectal exam (2%), and other (80%). Site of primary tumor was colonic in 51% and rectal in 49%. Synchronous malignant lesions were noted in 1%. Mucitious and signet cell histology was seen in 11% and 2%, respectively. Tumor grade distribution was grade 1 (2%), grade 2 (54%), grade 3 (34%), and grade 4 (7%). The stage distribution was stage 1 (13%), stage 11 (21%), stage 111 (32%), and stage IV (34%). To our knowledge, the current study is the largest cohort of young-onset CRC patients with no known genetic predisposition for disease. Most patients were symptomatic, had left-colon or rectal cancers and presented with more advanced stage disease. Our findings should promote increased awareness and the aggressive pursuit of symptoms in otherwise Young, low-risk patients, as these symptoms may represent an underlying colorectal malignancy.
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页码:259 / 263
页数:5
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