Hormonal Agents in Cancer Therapy
Antiestrogens, Aromatase Inhibitors, SERDs, Antiandrogens, Abiraterone, GnRH Analogues, Glucocorticoids & Recent Advances
Past RGUHS + DNB + MPMSU · 3
MPMSU2013
DNBDec '12
RGUHSApr '07
Introduction & principles
- Principle — the growth of breast and prostate carcinoma is hormone-dependent; interrupting steroid-hormone signalling delays recurrence and prolongs survival. Hormonal agents are not cytotoxic — they are cytostatic/palliative and must be given for prolonged periods (e.g. tamoxifen ≥5 years).
- Three strategies — (1) inhibit hormone production — GnRH analogues, aromatase inhibitors, abiraterone; (2) block hormone–receptor binding — SERMs, AR antagonists; (3) degrade the receptor — SERDs (fulvestrant).
- Receptors — ER, PR, AR and GR are ligand-activated nuclear-receptor transcription factors; blocking their activation silences gene networks driving tumour growth.
- Historical — breast cancer was the first neoplasm shown to respond to hormonal manipulation; Huggins (1941) showed androgens drive prostate cancer, establishing androgen-deprivation therapy (ADT) — Nobel Prize 1966.
- Predictive biomarker — ER+/PR+ breast tumours have a >60% chance of responding to endocrine therapy; ER–/PR– tumours do not respond. Response is lower when ER+ tumours are also HER2-amplified.
Continue reading
Hormones In Cancer Therapy
PharmaNotes Pro · LAQ
Sign in with your Google account. If you're already subscribed, the chapter unlocks immediately — otherwise, pick Monthly or Annual on the next step.