Profiling estrogen, progesterone, and androgen receptors in colorectal cancer in relation to gender, menopausal status, clinical stage, and tumour sidedness

Bassem Refaat; Akhmed Aslam; Shakir Idris; Ahmed H Almalki; Mofareh Y Alkhaldi; Hassan A Asiri; Riyad A Almaimani; Abdulrahman Mujalli; Faisal Minshawi; Sara A Alamri; Mona I AlHussain; Badee A Baltow; Mansour H Alqasmi; Ghaiyda T Basfar; Ohoud M Alosaimi; Ibrahim A Muhayya

doi:10.3389/fendo.2023.1187259

Profiling estrogen, progesterone, and androgen receptors in colorectal cancer in relation to gender, menopausal status, clinical stage, and tumour sidedness

Front Endocrinol (Lausanne). 2023 May 3:14:1187259. doi: 10.3389/fendo.2023.1187259. eCollection 2023.

Authors

Bassem Refaat¹, Akhmed Aslam¹, Shakir Idris¹, Ahmed H Almalki^{1

2}, Mofareh Y Alkhaldi^{1

3}, Hassan A Asiri^{1

4}, Riyad A Almaimani⁵, Abdulrahman Mujalli¹, Faisal Minshawi¹, Sara A Alamri⁶, Mona I AlHussain⁶, Badee A Baltow⁶, Mansour H Alqasmi⁷, Ghaiyda T Basfar^{1

7}, Ohoud M Alosaimi^{1

8}, Ibrahim A Muhayya³

Affiliations

¹ Laboratory Medicine Department, Faculty of Applied Medical Sciences, Umm Al-Qura University, Makkah, Saudi Arabia.
² Regional Laboratory and Central Blood Bank, Ministry of Health, Jizan, Saudi Arabia.
³ Laboratory And Blood Bank Department, Asir Central Hospital, Abha, Saudi Arabia.
⁴ Forensic Medicine Department, Health Affairs General Directorate in Assir, Abha, Saudi Arabia.
⁵ Biochemistry Department, Faculty of Medicine, Umm Al-Qura University, Makkah, Saudi Arabia.
⁶ Histopathology Department, King Abdullah Medical City, Makkah, Saudi Arabia.
⁷ Clinical Laboratories, Al-Noor Specialist Hospital, Makkah, Saudi Arabia.
⁸ Clinical Laboratories, Eradah and Mental Health Complex, Ministry of Health, Taif, Saudi Arabia.

Abstract

Background: Although estrogen (ERα/ERβ), progesterone (PGR), and androgen (AR) receptors are pathologically altered in colorectal cancer (CRC), their simultaneous expression within the same cohort of patients was not previously measured.

Methods: ERα/ERβ/PGR/AR proteins were measured in archived paired normal and malignant colon specimens (n =120 patients) by immunohistochemistry, and results were analyzed by gender, age (≤50 vs. ≥60 years), clinical stages (early-stage I/II vs. late-stage III/IV), and anatomical location (right; RSCs vs. left; LSCs). Effects of 17β-estradiol (E2), progesterone (P4), and testosterone alone or combined with the specific blockers of ERα (MPP dihydrochloride), ERβ (PHTPP), PGR (mifepristone), and AR (bicalutamide) on cell cycle and apoptosis were also measured in the SW480 male and HT29 female CRC cell lines.

Results: ERα and AR proteins increased, whilst ERβ and PGR declined markedly in malignant specimens. Moreover, male neoplastic tissues showed highest AR expression, whilst ERβ and PGR weakest alongside ERα strongest expression was seen in cancerous tissues from women aged ≥60 years. Late-stage neoplasms also revealed maximal alterations in the expression of sex steroid receptors. By tumor location, LSCs disclosed significant elevations in ERα with marked declines in PGR compared with RSCs, and ERα strongest alongside PGR weakest expression was detected in advanced LSCs from women aged ≥60 years. Late-stage LSCs from females aged ≥60 years also showed weakest ERβ and strongest AR expression. In contrast, male RSC and LSC tissues exhibited equal ERβ and AR expression in all clinical stages. ERα and AR proteins also correlated positively, whereas ERβ and PGR inversely, with tumor characteristics. Concomitantly, E2 and P4 monotherapies triggered cell cycle arrest and apoptosis in the SW480 and HT29 cells, and while pre-treatment with ERα-blocker enhanced the effects of E2, ERβ-blocker and PGR-blocker suppressed the E2 and P4 anti-cancer actions, respectively. In contrast, treatment with the AR-blocker induced apoptosis, whilst co-treatment with testosterone hindered the effects.

Conclusions: This study advocates that protein expression of sex steroid receptors in malignant tissues could represent prognostic markers, as well as hormonal therapy could provide an alternative strategy against CRC, and their efficacies could be dependent on gender, clinical stage, and tumor location.

Keywords: apoptosis; bicalutamide; cell cycle; estrogen receptor-α (ERα); estrogen receptor-β (ERβ); left-right dichotomy; mifepristone; testosterone.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Colorectal Neoplasms* / drug therapy
Estrogen Receptor alpha* / metabolism
Estrogen Receptor beta* / metabolism
Estrogens / pharmacology
Female
Humans
Male
Menopause
Progesterone / pharmacology
Receptors, Androgen* / metabolism
Receptors, Estrogen / metabolism
Receptors, Progesterone* / metabolism
Testosterone / pharmacology

Substances

Estrogen Receptor alpha
Estrogen Receptor beta
Estrogens
Progesterone
Receptors, Androgen
Receptors, Estrogen
Testosterone
Receptors, Progesterone

Grants and funding

This work was supported by the Deputyship for Research & Innovation, Ministry of Education in Saudi Arabia [Grant Code: IFP22UQU4320045DSR101]. The funding organization was not involved in the design of the study; the collection, analysis, and interpretation of data; writing the report; and did not impose any restrictions regarding the publication of the report.