Figure 3 The mean percentage of

the

Figure 3 The mean Epacadostat cost percentage of

the positively immunostained cells for p53, p16, bcl-2, ki-67, c-myc, Rb, and EGFR in tumor tissue sections of SBT in relation to (A) histopathology; SCC and TCC. (B) Grade of the tumor; high and low grades. (C) Invasiveness of the tumor; invasive and non-invasive (D) Stage of cancer; late (stages VI and III) and early stages (stages I and II). (E) Presentation of the disease; first presentation and recurrent. Regarding NSBT, only p53 and c-myc were clearly associated with SCC while EGFR, unlike in SBT, was associated with TCC (P < 0.05) (Figure. 4-A). All studied markers were higher in high grade tumors than in low grade and p16 was very low in high grade tumors (P < 0.05) (Figure. 4-B). Bcl-2, c-myc, and EGFR were higher in invasive than in non-invasive tumors while p16 and Rb, unlike in SBT, were lower in invasive selleck than in non-invasive (P < 0.05) (Figure. 4-C). Ki-67, c-myc, and EGFR were higher in late stages

of the disease than MDV3100 datasheet early stages while p16 and Rb were lower in late than early stages (P < 0.05) (Figure. 4-D). Bcl-2 was higher and p16 and Rb were lower in recurrent than in first presentation (P < 0.05) (Figure. 4-E). Figure 4 The mean percentage of the positively immunostained cells for p53, p16, bcl-2, ki-67, c-myc, Rb, and EGFR in tumor tissue sections of NSBT in relation to (A) histopathology; SCC and TCC. (B) Grade of the tumor; high and low grades. (C) Invasiveness of the tumor; invasive and non-invasive.

(D) Stage of cancer; late (stages VI and III) and early stages (stages I and II). (E) Presentation of the disease; first presentation and recurrent. The behavior of the studied markers Silibinin in SBT and NSBT was sometimes similar and sometimes different in relation to the clinicopathological criteria. Collectively, in both SBT and NSBT, the similar behavior of the studied markers was as follows; a) p53 was associated with SCC. b) p53, bcl-2, and c-myc were higher in high grade tumors. c) Bcl-2, c-myc, and EGFR were higher in invasive than non-invasive tumors. d) P16 and Rb were lowered in late stages of the disease (III and IV) while c-myc was higher. e) Rb and p16 were lowered in the recurrent presentation. On the other hand, the main lines of difference in the expression of the studied markers between SBT and NSBT were briefly as follows: a) In SBT, bcl-2, Rb, and EGFR were associated with SCC while in NSBT c-myc was associated with SCC and EGFR was associated with TCC. b) ki-67, Rb, and EGFR were higher in high grade tumors in NSBT rather than SBT. c) ki-67 was higher in invasive than in non-invasive tumors in SBT while p16 and Rb were lower in invasive than in non-invasive in NSBT. d) EGFR and ki-67 were higher in late stages of the disease in NSBT only. e) Bcl-2 in NSBT was higher in recurrent cases than first time presentation.

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