Immunohistochemical predictors of recurrent ovarian endometriomas after laparoscopic surgery

E Yu Pshenichnyuk; Pshenichnyuk E.Yu. Pshenichnyuk; A V Asaturova; L V Adamyan; N V Zaytsev

doi:10.17116/patol201880414

Immunohistochemical predictors of recurrent ovarian endometriomas after laparoscopic surgery

E Yu Pshenichnyuk, Pshenichnyuk E.Yu. Pshenichnyuk, A V Asaturova, L V Adamyan, N V Zaytsev

Arkhiv patologii · 2018 · vol. 80(4) , pp. 14 · doi:10.17116/patol201880414 · PMID:30059067 · W2886561314

article OA: closed CC0 ⤵ 1 in-corpus citation

View on OpenAlex View on PubMed View at publisher

⚙ AI-generated summary by claude@2026-06, 2026-06-08 ⓘ

Recurrent ovarian endometriomas showed decreased Ki-67, NF-kβ p65, and COX-2 expression, but increased β-catenin and PR-α expression compared to non-recurrent cases.

One-sentence paraphrase of the abstract; not a substitute for reading it. No clinical advice. How this works

Abstract

OBJECTIVE: To investigate the expression of proliferation and apoptotic factors (Ki-67, Bcl-2), inflammatory factors (NF-kβ p65, COX-2), adhesion factors (β-catenin), estrogen (ER-α) and progesterone receptors (PR-α) in ovarian endometrioma (OE) in patients with recurrent OE by an immunohistochemical assay. SUBJECT AND METHODS: This investigation enrolled 48 reproductive-aged patients with OE. According to the course of the disease during a follow-up period of 1.5 years after surgical treatment, the biomaterial obtained from the examined patients was divided into two groups: 1) an OE capsule from 19 patients with recurrent OE (a study group); 2) an OE capsule from 28 patients without recurrent OE (a comparison group). This investigation used histological and immunohistochemical examinations. The histological analysis of the OE capsule was performed following a standard procedure. Their immunohistochemical analysis was carried out using the Tissue-Tek Quick-Ray kit that allows the preparation of paraffin blocks with a large number of tissue samples (tissue microarrays). Antibodies to Ki-67 (clone 30-9, VENTANA), Bcl-2 (clone 124, VENTANA), NF-kβ p65 (clone p65, 'Spring Bioscience Corp.'), COX-2 (clone CX-294, Agilent), β-catenin (clone 14, VENTANA), ER-α (clone SP1, VENTANA), and PR-α (clone 1E2, VENTANA) were also employed in the investigation. The specimens were prepared according to a standard protocol using a Ventana Ultra immunohistostainer. Positive and negative controls were used to correctly carry out immunohistochemical tests. Statistical analysis was performed using the applied statistical analysis programs Statistica 10.0 and Microsoft Excel. RESULTS: The patients with recurrent OE had a significantly decreased expression of Ki-67 (2.86% vs. 9.69%; р=0.044) in the epithelial component of the OE capsule; a significantly lower expression of NF-kβ p65 (2.54 vs. 3.5; р=0.0082) and СОХ-2 (0.231 vs. 1.381; р=0.0025) in the stromal component of the OE capsule, a significantly increased expression of β-catenin (2.5 vs. 1.59; р=0.017) in the stromal component of the OE capsule; a significantly increased expression of PR-α (188.46 vs. 71.15; р=0.028) in the epithelial component of an OE capsule. The expression of ER-α (stromal component, 266 vs. 256.84; p=0.48; epithelial component, 251.54 vs. 233.85, p=0.82) and Bcl-2 (stromal component, 0.33 vs. 0.25; p=0.85; epithelial component, 0.944 vs. 0.625; p=0.31) in the OE capsule is not statistically significantly different between the study patient groups. CONCLUSION: The immunohistochemical difference in the expression of a number of the markers under study can serve as the basis for a further investigation of these markers as predictors of recurrent OE after surgical treatment. Further investigations of these factors will also be able to examine the molecular mechanisms underlying the pathogenesis of recurrent OE, which will make it possible to affect these mechanisms in order to eliminate the fundamental causes of a recurrence of this disease.

My notes (saved in your browser only)

Condition tags

mesh:D004715endometrioma

MeSH descriptors

Biomarkers Endometriosis Ovary Prognosis Adult beta Catenin beta Catenin Biomarkers Cyclooxygenase 2 Cyclooxygenase 2 Endometriosis Endometriosis Endometriosis Female Gene Expression Regulation Gene Expression Regulation Humans Immunohistochemistry Ki-67 Antigen Ki-67 Antigen

Citation neighborhood

Papers in the corpus that this work cites (lower rings, blue) and that cite this one (upper rings, green). Dot size scales with the paper's in-corpus citation count — bigger dot = more influential within the endo/adeno field. Click a dot to open that paper. [ expand to 2 hops ] — adds papers reached through this work's immediate citers/citees. Heavier; up to 60 extra dots.

References (26)

Cited by (1)

Risk factors for recurrence of endometrioid ovarian cysts after combined treatment 2022

Source provenance

europepmc: last seen: 2026-06-04T01:30:01.192114+00:00
openalex: last seen: 2026-06-10T16:23:13.998983+00:00
pubmed: last seen: 2026-05-13T22:19:37.156494+00:00
unpaywall: last seen: 2026-06-06T02:00:05.402940+00:00

License: CC0 · commercial use OK

[1] Aberrant DNA methylation status of endometriosis: Epigenetics as the pathogenesis, biomarker and therapeutic target via openalex

[2] Analysis of cyclooxygenase-2 (COX-2) expression in different sites of endometriosis and correlation with clinico-pathological parameters via openalex

[3] Cyclooxygenase-2 overexpression in ovarian endometriomas is associated with higher risk of recurrence via openalex

[4] Cyclooxygenase-2 Regulates Survival, Migration, and Invasion of Human Endometriotic Cells through Multiple Mechanisms via openalex

[5] Dienogest increases the progesterone receptor isoform B/A ratio in patients with ovarian endometriosis via openalex

[6] Endometriosis: hormone regulation and clinical consequences of chemotaxis and apoptosis via openalex

[7] Estrogen and progesterone receptors in endometriotic tissue and endometrium: comparison according to localization and recurrence via openalex

[8] Evaluation of the Ki-67 Proliferation Index and Urocortin Expression in Women with Ovarian Endometriomas via openalex

[9] Expression and significance of ERβ and TrkB in endometriosis via openalex

[10] Hypoxia Promotes Invasion of Endometrial Stromal Cells via Hypoxia-Inducible Factor 1α Upregulation-Mediated β-Catenin Activation in Endometriosis via openalex

[11] Increased cyclooxygenase-2 expression is associated with better clinical outcome in patients submitted to complete ablation for severe endometriosis via openalex

[12] Nuclear Factor-κB (NF-κB): An Unsuspected Major Culprit in the Pathogenesis of Endometriosis That Is Still at Large? via openalex

[13] ‘Omic’ high-throughput technologies in research on pathogenesis of endometriosis: a Review via openalex

[14] Post-operative endometriosis recurrence: a plea for prevention based on pathogenetic, epidemiological and clinical evidence via openalex

[15] Postoperative Medical Therapy After Surgical Treatment of Endometriosis: From Adjuvant Therapy to Tertiary Prevention via openalex

[16] Prevention of the recurrence of symptom and lesions after conservative surgery for endometriosis via openalex

[17] Recurrence of ovarian endometrioma after laparoscopic excision: Risk factors and prevention via openalex

[18] Risk factors and biomarkers for the recurrence of ovarian endometrioma: about the immunoreactivity of progesterone receptor isoform B and nuclear factor kappa B via openalex

[19] Study of gene expressions in the eutopic endometrium of women with endometrioid ovarian cysts via openalex

[20] The detection rate and the structure of pathological changes of the endometrium in women of reproductive age with endometriosis via openalex

[21] Towards an understanding of the molecular mechanism of endometriosis: unbalancing epithelial-stromal genetic conflict via openalex

[22] W2098361539 via openalex

[23] W2146933137 via openalex

[24] W2061665035 via openalex

[25] W4247489276 via openalex

[26] W2416443245 via openalex