Clinical Trial Details
— Status: Not yet recruiting
Administrative data
| NCT number |
NCT04891731 |
| Other study ID # |
SunYatsenU2H-LQ5 |
| Secondary ID |
|
| Status |
Not yet recruiting |
| Phase |
|
| First received |
|
| Last updated |
|
| Start date |
May 2021 |
| Est. completion date |
September 2023 |
Study information
| Verified date |
May 2021 |
| Source |
Sun Yat-Sen Memorial Hospital of Sun Yat-Sen University |
| Contact |
Jingna Lin, MD |
| Phone |
18819430558 |
| Email |
229320178[@]qq.com |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Observational
|
Clinical Trial Summary
Leuprorelin, a LHRH agonist, acts as a potent inhibitor of gonadotropin secretion and is
commonly used for the treatment of hormone-responsive prostate cancer, premenopausal HR+
breast cancer, endometriosis and uterine fibroids. It is currently available in 1M, 3M, 6M
for subcutaneous administration. Initially administration would stimulate an increase in LH
and FSH, causing a transient increase of E2 in 2-4 weeks. Continuous administration results
in a subsequent decrease in E2 levels, as a result of decreased levels of luteinizing LH and
FSH. After stopping injection, ovarian function could gradually recover. Adverse events
related to leuprorelin include flushing, mood swings and urogenital symptoms.
At present, the treatment of premenopausal breast cancer mainly includes 1M and 3M GnRHa.
Leuprorelin 11.25mg dosage form is currently the only 3M GnRHa in China that has gotten
breast cancer indications. The use of 3M GnRHa could improve patients' compliance and reduce
injection discomfort. However, previous studies about GnRHa alone or in combination with TAM
or AIs usually used 1M GnRHa. There have been few studies reporting the suppression effects
of E2 levels and clinical outcome with leuprorelin 3M in combination with TAM or AIs.
Description:
Background:
There are some differences in the age of onset of breast cancer, histopathological types, and
treatment methods between Asians and non-Asians. Incidence peaks at age 40-50 in Asian women,
with more than half of premenopausal patients, but 65-70 years in US women, most of which are
postmenopausal[1]. Besides, compared with Americans, Asian women younger than 50 have a
higher prevalence of luminal A breast cancer and less basal-like subtype. Therefore, the
application of OFS has always been the focus for the treatment of premenopausal women with
HR+ breast cancer in Asia.
OFS therapy includes oophorectomy, ovarian radiation, and the use of GnRHa. Several studies
have shown that the use of GnRHa in premenopausal women can achieve similar efficacy to
oophorectomy and ovarian radiation therapy. As GnRHa has the advantages of non-invasiveness
and reversibility, it has gradually replaced oophorectomy and ovarian radiation, and has
become the main method of OFS in premenopausal women with HR+ breast cancer. Meanwhile, GnRHa
in combination with TAM or AIs is increasingly used for premenopausal HR+ breast cancer
patients. Previous studies have revealed that GnRHa alone or in combination with TAM or AIs
has shown effective estrogen suppression and certain survival benefits for most patients with
breast cancer. In addition, the 5-year follow-up results of the TEXT / SOFT study in 2014
showed that compared with OFS + TAM, OFS + AI treatment significantly improved DFS, prolonged
cancer-free survival time and distant recurrence-free metastasis[8, 9]. The 9-year follow-up
results of the TEXT / SOFT study in 2019 indicated that OFS + AI versus OFS + TAM or TAM
single drugs, years of distant recurrence risk in patients with high risk of recurrence have
an absolute benefit rate of 10-15 %, Intermediate risk is 4-5%, low-risk benefit is not
obvious. In 2019, the ABCCG reviewed ESO-ESMO and St. Gallen's treatment recommendations for
HR+/ Her-2 negative breast cancer in premenopausal women, discussed controversial issues and
pointed out that patients with low recurrence risk can be treated with TAM alone. For
patients with high risk of recurrence, chemotherapy + OFS + AI should be given. It indicates
that not all premenopausal HR+ patients with early breast cancer need auxiliary OFS, and more
clinical trials on OFSin premenopausal HR + patients are necessary and worthwhile.
Leuprorelin, a LHRH agonist, acts as a potent inhibitor of gonadotropin secretion and is
commonly used for the treatment of hormone-responsive prostate cancer, premenopausal HR+
breast cancer, endometriosis and uterine fibroids. It is currently available in 1M, 3M, 6M
for subcutaneous administration. Initially administration would stimulate an increase in LH
and FSH, causing a transient increase of E2 in 2-4 weeks. Continuous administration results
in a subsequent decrease in E2 levels, as a result of decreased levels of luteinizing LH and
FSH. After stopping injection, ovarian function could gradually recover. Adverse events
related to leuprorelin include flushing, mood swings and urogenital symptoms.
At present, the treatment of premenopausal breast cancer mainly includes 1M and 3M GnRHa.
Leuprorelin 11.25mg dosage form is currently the only 3M GnRHa in China that has gotten
breast cancer indications. The use of 3M GnRHa could improve patients' compliance and reduce
injection discomfort. However, previous studies about GnRHa alone or in combination with TAM
or AIs usually used 1M GnRHa. There have been few studies reporting the suppression effects
of E2 levels and clinical outcome with leuprorelin 3M in combination with TAM or AIs.
To further investigate the suppression effects of E2 levels of 3M GnRHa, we conducted a
single-arm, prospective clinical observational study evaluating the efficacy and safety of
adjuvant therapy with leuprorelin 3M in combination with TAM or AIs in premenopausal HR+
breast cancer.
