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Testosterone and Androgen Receptor in Cancers with Significant Sex Dimorphism in Incidence Rates and Survival
1
Tripill Biotechnolgy, Corp., Chapel Hill, NC 27516, USA
2
Department of Pharmacy and Pharmaceutical Sciences, St. Jude Children’s Research Hospital, Memphis, TN 38105, USA
3
Department of Preventive Medicine, College of Medicine, University of Tennessee Health Science Center, Memphis, TN 38105, USA
4
Department of Medicine, College of Medicine, University of Tennessee Health Science Center, Memphis, TN 38105, USA
5
Department of Dermatology, College of Medicine, University of Tennessee Health Science Center, Memphis, TN 38105, USA
*
Author to whom correspondence should be addressed.
Cancers 2025, 17(21), 3414; https://doi.org/10.3390/cancers17213414
Submission received: 7 September 2025
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Revised: 16 October 2025
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Accepted: 17 October 2025
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Published: 23 October 2025
(This article belongs to the Special Issue Feature Paper in Section ‘Cancer Epidemiology and Prevention’ in 2025)
Simple Summary
Sex differences play an important role in how certain cancers develop and progress. This study reviewed patterns of cancer incidence and survival between men and women, focusing on tumors of the esophagus, bladder, head and neck, lung, liver, kidney, stomach, and skin melanoma. We explored how male sex hormones (mainly testosterone) and the androgen receptor (AR) may influence cancer risk and outcomes. In some cancers, higher AR activity is linked to worse survival, suggesting that therapies targeting AR could help certain patients. However, the relationship between hormones and cancer is complex and not fully understood. More research is needed to clarify these effects and to develop treatments that consider biological sex as a factor in cancer care.
Abstract
Several major cancer types exhibit significant sex dimorphism in incidence and survival. Whether and how sex as a biological factor impacts tumorigenesis, progression, and survival warrants full investigation, as such knowledge may lead to novel, precise prevention and treatment strategies. We reviewed epidemiological and molecular data on sex differences in cancers of the esophagus, bladder, head and neck, lung, liver, kidney, stomach, and skin melanoma, as well as the potential role of androgens and androgen receptor (AR) activity in these cancers. The potential molecular mechanisms are briefly discussed. Elevated testosterone (T) levels seemed to be associated with increased liver cancer and cutaneous melanoma incidences, and with reduced esophageal cancer risk. AR activity does not always correlate with T levels in tumorigenesis and progression. Higher AR expressions are associated with poorer survival in ESCC, whereas the role of AR in the survival of HNSCC and melanoma patients is inconsistent. The molecular impact of AR in liver cancer, kidney cancer, melanoma, and lung cancer is controversial. However, AR is likely to promote tumor growth and/or progression in esophagus, bladder, head and neck, and stomach cancers, and thus is associated with poor survival. Patients diagnosed with a tumor in this latter group could potentially benefit from therapeutic approaches targeting AR. Overall, the research on sex hormone androgens and AR in these cancers is limited. Further research is needed to determine a possible U-shaped relationship of T with cancer risk, and to decipher the role of testosterone and AR in some of these tumors to facilitate our understanding of sex dimorphism and to explore novel T/AR-based treatment options.
Keywords:
testosterone; androgen receptor; cancer; sex dimorphism
