Abstract: Objective To study on the expressions and clinical significance of tumor-associated genes in human rectal cancers and corresponding normal para-cancer rectal mucosa. Methods 54 cases of human rectal cancer and 40 cases of para-cancer mucosa were collected and made into two tissue microarrays which containing 54 dots and 130 dots respectively. Expressions of p53, cyclinD1, bcl-2, β-catenin, c-myc, COX-2 and nm23-h1 proteins were detected by immunohistochemical staining to these tissue microarrays. Results Significant differences were found among rectal cancers and benign para-cancer mucosa according to the expressions of p53, cyclinD1, bcl-2, β-catenin, c-myc, COX-2 and nm23-h1 (P<0.05). Furthermore, the positive correlation of expressions of p53 with bcl-2 and β-catenin with c-myc were also found respectively in this study (r=0.332, P=0.001 and r=0.447,P=0.000). Expression of p53, c-myc and COX-2 had no correlations of expression of p53, c-myc and COX-2 with clinicopathological data of these rectal cancer tissues. However, we found that β-catenin expression was correlated with patient years which showed proportion of β-catenin expression in patients more than 60 years old was higher than that in patients less than 60. Although β-catenin and bcl-2 expressions had relationships with historical grades, cancer tissues in this cohort with over-expression of β-catenin or bcl-2 were less facility to differentiate to advanced grade and invasive to focus and distance. Expression of cyclinD1 has no correlation with other clinicopathological parameters but clinical stages (P=0.039). In addition to these results, the relationships of nm23-h1 expression and tissue differentiation, distance metastasis and duke's stages were found. Conclusion Abnormal expressions of p53, cyclinD1, bcl-2, β-catenin, c-myc, COX-2 and nm23-h1, specially over-expressions of p53, cyclinD1and bcl-2 may contribute to the early diagnosis in human rectal cancer. Furthermore, aberration of cyclinD1 may involve in rectal cancer progression. Distortion of nm23-h1 may have potent role in cancer metastasis so that prognosis may increase while adjuvant therapy was used early in patients with low-expression of nm23-h1.