Introduction: Prostate cancer is among the most common malignant diseases in men and is one of the leading health problems of older men. The Croatian Cancer Registry ranked prostate cancer first in terms of frequency and second in terms of mortality from malignant diseases in men. One of the preferred standard forms of treatment for localized prostate cancer is radical radiotherapy. The effectiveness of radiotherapy treatment is limited by toxic side effects. In addition, cancer cells develop mechanisms of radioresistance associated with DNA repair, inhibition of apoptosis or changes in the cell cycle. In the literature biomarkers that participate in those cellular mechanisms (p53, bcl-2, NF-kb, Cripto-1) have been poorly correlated with clinical and pathological parameters (PSA value, Gleason score, grade and prognostic group, stage bojesti, proliferative activity index-Ki67) in patients treated with radiotherapy. Objective: To validate the immunohistochemical expression of: p53, bcl-2, NF κB, Cr -1 in tissue microarrays of prostate cancer patients treated with radical radiotherapy. To determine the relationship between immunohistochemical parameters and clinical-pathological characteristics and the relationship between clinical-pathological characteristics and immunohistochemical biomarkers with radiotherapy treatment outcomes, in the form of disease progression (appearance of metastases), disease-free survival and overall survival. Material and procedures: 90 patients with prostate cancer treated with radical radiotherapy (total dose 64 Gy) and followed for at least 48 months, were selected by reviewing the medical data of the KBC Rijeka Tumor Clinic. Patients included in this retrospective study had tumors confined to the prostate or locally advanced disease who had a pathohistological specimen adequate for immunohistochemical analysis and those with complete medical data. Pathohistological material of those patients was selected at the Department of Pathology of KBC Rijeka for the creation of tissue microarrays, which were then immunohistochemically stained with antibodies for p53, bcl-2, NFκB and Cr-1. The progression of the disease was determined by the appearance of metastases, and the data obtained from the pathologist by analizing the percentage of positive immunohistochemical staining on 500 cells were processed using standard statistical methods. Results: We confirmed the already well-known statistically significant association of disease stage with Gleason score and prognostic group. A higher stage of the disease means, on average,an increased Gleason score and a higher prognostic group. Gradus group was not only related to stage, while a statistically significant positive correlation was found with other parameters. The expression of p53 was statistically significantly related to the stage of the disease and the grade group, whereby the expression in the first stage and the lower grade group was lower than the expression in the third stage. The expression of nfκb was only related to the prognostic group, where in prognostic groups 1 and 2 there was a statistically significantly lower expression than in groups 4 and 5. The logrank test showed that the grade group was associated with survival, and the risk ratio analysis was statistically significant the difference between the first and second and first and fifth grade groups. Also, the statistically significant association between disease progression and the expression of nfκb and Ki67 determined the best predictive potential, with nfκB emphasizing sensitivity and Ki67 specificity. The expression of Cr-1 was not statistically significantly related to any of the observed parameters, although in the analysis of disease progression it showed high sensitivity, while p53 and bcl2 had high specificity. Multivariate analysis in relation to the five-year period without disease progression showed a significant predictive value of the immunohistochemical parameters p53, Nfkb, bcl by assessing the levels of these three biomarkers together, but not individually. As expected, survival was related to clinicopathological parameters and tumor proliferative activity, i.e. Ki67 immunoexpression. Conclusion: The results of the study confirmed the impact of the expression of p53, bcl-2, nfκb, Cr -1 on the outcome of radiotherapy treatment. Biomarkers nfκb and Ki67 showed the best predictive potential of disease progression. All validated immunohistochemical parameters confirmed a certain association with survival, but only the Ki67 proliferation index was statistically significant. By constructing a numerical index based on all clinical-pathological and immunohistochemical parameters, a threshold score of >21 or more was established as an indicator of a significant risk for progression. In the case of a numerical index greater than 21, the patient is at greater risk of disease progression after completion of radiotherapy treatment and should be monitored more carefully. Key words: an increased Gleason score and a higher prognostic group. Gradus group was not only related to stage, while a statistically significant positive correlation was found with other parameters. The expression of p53 was statistically significantly related to the stage of the disease and the grade group, whereby the expression in the first stage and the lower grade group was lower than the expression in the third stage. The expression of nfκb was only related to the prognostic group, where in prognostic groups 1 and 2 there was a statistically significantly lower expression than in groups 4 and 5. The logrank test showed that the grade group was associated with survival, and the risk ratio analysis was statistically significant the difference between the first and second and first and fifth grade groups. Also, the statistically significant association between disease progression and the expression of nfκb and Ki67 determined the best predictive potential, with nfκB emphasizing sensitivity and Ki67 specificity. The expression of Cr-1 was not statistically significantly related to any of the observed parameters, although in the analysis of disease progression it showed high sensitivity, while p53 and bcl2 had high specificity. Multivariate analysis in relation to the five-year period without disease progression showed a significant predictive value of the immunohistochemical parameters p53, Nfkb, bcl by assessing the levels of these three biomarkers together, but not individually. As expected, survival was related to clinicopathological parameters and tumor proliferative activity, i.e. Ki67 immunoexpression. Conclusion: The results of the study confirmed the impact of the expression of p53, bcl-2, nfκb, Cr -1 on the outcome of radiotherapy treatment. Biomarkers nfκb and Ki67 showed the best predictive potential of disease progression. All validated immunohistochemical parameters confirmed a certain association with survival, but only the Ki67 proliferation index was statistically significant. By constructing a numerical index based on all clinical-pathological and immunohistochemical parameters, a threshold score of >21 or more was established as an indicator of a significant risk for progression. In the case of a numerical index greater than 21, the patient is at greater risk of disease progression after completion of radiotherapy treatment and should be monitored more carefully.