TY - JOUR ID - TI - Diagnostic value of immunohistochemical panel (Cytokeratin CK 7, Cytokeratin CK20, High molecular weight cytokeratin HMWCK (clone CK34βE12) and Prostatic specific antigen (PSA) in differentiation between poorly differentiated prostatic and urothelial carcinoma AU - Ikram A. Hasan AU - Hiba A. Gaidan AU - Methaq M. Al-kaabi PY - 2018 VL - 11 IS - 1 SP - 7 EP - 13 JO - Iraqi Journal of Cancer and Medical Genetics المجلة العراقية للسرطان والوراثة الطبية SN - 20786123 23135379 AB - Background: Prostatic adenocarcinoma may spread to bladder or vice versa, this is because of the anatomical proximity ofthese two organs. The differentiation between these two tumors is critical for therapeutic and prognostic implication.Aim of study: Evaluate the usefulness of a panel of immunohistochemical markers (CK7, CK20, HMWCK34 βE12 andPSA) in differentiation between challenging cases of high grade urothelial and poorly differentiated prostatic carcinoma withmorphological overlapping.Material and methods: A total of 40 cases (20 cases poorly differentiated prostatic adenocarcinoma and 20 cases high gradeurothelial carcinoma) were collected from archive of teaching laboratory of Al Yarmouk teaching hospital and private laboratoriesfor the period from January 2015 to July 2017.All formalin fixed paraffin embedded tissue block were stained immunohistochemicallywith a panel of marker (CK7, CK20, HMWCK34 βE12 and PSA) and scoring was performed.Results: For prostatic adenocarcinoma, 17 out 20 (85%) were positive for PSA, while only two cases (10%) of urothelial carcinomacases showed weak and focal staining for this marker (the pvalue was <0.0001). In contrast, 16 out of 20(80%) of theurothelial carcinoma cases were positive for CK34βE12 in comparison to only one case (5%)of prostatic carcinoma showedpositive expression for this marker (the p value was highly significant <0.0001).Regarding CK7and CK20: combined expression of both markers was noticed in 17 cases (85%) of urothelial carcinomacompared to only 2 cases(10%) of prostatic adenocarcinoma and the difference was highly significant(p value <0.0001). negativeexpression for both markers was noticed in 18 cases (90%) of prostatic adenocarcinoma compared to only 2 cases (10%)of urothelial carcinoma and the difference was highly significant( p value < 0.0001).CK7 positivity alone was noted in 17cases(85%) of urothelial carcinoma while only 2 cases (10%) of prostatic carcinoma show positivity for this marker and the pvalue was highly significant (p value < 0.0001).18 cases (90%) of urothelial carcinoma showed positive expression for CK20alone compared to only to 3 cases (15%) of prostatic carcinoma (p value < 0.0001).Conclusion: Using CK7 or CK20 alone will not be helpful for differentiation between prostatic carcinoma and high gradeurothelial carcinoma, while combined expression of both markers(CK7 and CK20) is very useful in ruling out carcinoma ofthe prostate, since, it is very rare for both markers to show positive expression in prostatic carcinoma.In difficult cases thatshow negative expression of both marker, CK34βE12 remain the most valuable marker for urothelial origin while, PSA immunohistochemicalmarker remains the most helpful marker to prove the prostatic origin of metastatic carcinoma.

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