The relationship of immunohistochemical SOX-2 staining with histopathological diagnosis in patients with abnormal colposcopic findings

This study aimed to analyze immunohistochemical staining and pathological data in cervical intraepithelial neoplasia (CIN) and squamous cell cervical carcinoma (SCC) with abnormal colposcopic findings. A histopathological evaluation of 45 low-grade squamous lesions (LSILs), 177 high-grade squamous l...

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Veröffentlicht in:Histochemistry and cell biology 2023-12, Vol.160 (6), p.555-561
Hauptverfasser: Atıgan, Ayhan, Kılıç, Derya, Karakaya, Yeliz Arman, Gök, Soner, Güler, Ömer Tolga
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Sprache:eng
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Zusammenfassung:This study aimed to analyze immunohistochemical staining and pathological data in cervical intraepithelial neoplasia (CIN) and squamous cell cervical carcinoma (SCC) with abnormal colposcopic findings. A histopathological evaluation of 45 low-grade squamous lesions (LSILs), 177 high-grade squamous lesions (HSILs) and 16 SCC biopsy materials from existing slides was obtained from blocks obtained from the archive. In addition, SOX-2 immunohistochemical staining was evaluated. The mean age of the HSIL group was 43.20 ± 8.97 years, younger than the mean age of the LSIL group of 51.62 ± 9.64 years ( p  = 0.000). There was no difference between the groups regarding the method of biopsy ( p  > 0.05). Endocervical gland involvement was not observed in the LSIL group, but was observed in 66 (37.3%) biopsy materials in the HSIL group ( p  = 0.000). There was a difference between the groups in terms of the level of CIN at the surgical margin ( p  = 0.000). Ki-67, SOX-2 staining percentage and p16INK4a positivity were higher in the HSIL group than in the LSIL group (respectively, 67.57 ± 19.10 vs. 14.62 ± 7.11, p  = 0.000; 27.72 ± 31.56 vs. 10.09 ± 15.38, p  = 0.003; 66 (82.5%) vs. 8 (44.4%), p  = 0.001). While there was no difference in SOX-2 intensity between the HSIL and LSIL groups ( p  > 0.05), it was statistically significantly higher in the SCC group ( p  = 0.000), as was the percentage of SOX-2 ( p  = 0.000). We have shown that p16INK4a and SOX-2 staining is useful, in addition to Ki-67 immunostaining, which is widely used for SCC, which is one of the preventable cancer types. In addition, SOX-2 may provide a glimmer of hope in the development of SCC treatment modalities, especially since it is aggressively elevated in SCC rather than CIN lesions.
ISSN:0948-6143
1432-119X
DOI:10.1007/s00418-023-02230-4