Breast Cancer Clinical Trial
Official title:
Combination of CAF and Simvastatin Improves Response to Neoadjuvant Chemotherapy and Increases Tumor-Free Margin in Locally Advanced Breast Cancer: A Randomized, Double-Blind, Placebo-Controlled Trial
Introduction: Neoadjuvant chemotherapy (NACT) has been the standard therapy for treating
patients with locally advanced breast cancer (LABC). Doxorubicin-based regimen showed a
clinical response for 70-80%. However, the cardiotoxicity from it was not tolerable.
Simvastatin acts synergistically with doxorubicin against MCF-7 cells, through downregulation
of the cell cycle or induction of apoptosis. Also, it alleviates doxorubicin cardiotoxicity
by attenuating ER stress and activating the Akt pathway. Hmgcris a new pathway mediating
doxorubicin-induced cell death, and cholesterol control drugs combined with doxorubicin could
enhance efficacy and reduce side effects. This study is conducted to see the combination
simvastatin and CAF would increase the NACT response and surgical margin of LABC patients.
Methods: This study was a double-blind, randomized placebo-controlled trial, conducted in dr.
Cipto Mangunkusumo General Hospital and Koja General Hospital. A total of 70 LABC patients
were assessed for eligibility. Patients received either a combination of CAF-Simvastatin (40
mg/day) or CAF-Placebo. The biopsy was taken pre-NACT to make the histopathological diagnosis
and examine the expression of HMG-CoA Reductase (Hmgcr) and P-glycoprotein (P-gp). Patients
were evaluated for the clinical response after 3 cycles. If the response was positive,
patients will proceed to surgery. Then, the post-operative specimen will be reviewed for the
pathological response. However, if it was a negative response, patients will be given 2nd
line NACT.
Backgrounds Neoadjuvant chemotherapy (NACT) which is followed by surgery is now a standard
therapy in the local advanced breast cancer (LABC) since it was introduced 50 years ago,
increasingly being used in early-stage LABC patients. Some NACT studies in RSCM use a
doxorubicin-based regimen, giving a 70-80% partial response, but do not require a complete
response both clinically and pathologically. The NACT response was 80% with a complete
clinical response of 36%. The complete pathological response obtained after NACT is the
prognosis of a replacement marker both overall and disease-free survival in the LABC. The
purpose of giving NACTis to increase tumor resectability and de-escalation surgery and kill
micrometastasis which will increase the length of disease-free and life expectancy of the
patient. New tumor margins causing post-NACT tumor shrinkage can be used as surgical margins.
Doxorubicin-based chemotherapy is the most commonly given chemotherapy for NACT as well as
entering the first line of the National Formulary. However, side effects are limited from
drug resistance side effects that can cause cardiomyopathy and heart failure. One of the
factors that influence doxorubicin resistance is the presence of efflux pumps such as
P-glycoprotein (P-gp) on the cell surface. While the effects of toxicity arise due to the
formation of reactive oxygen species (ROS) and the presence of free radicals. Efforts to
improve the efficacy of the combination of chemotherapy currently being used with targeted
therapies such as anti-HER-2 and bevacizumab, but have a high enough toxicity and are
expensive and not included in ForNas. Likewise, some drugs that have been tested in vitro as
P-gp inhibitors/modifiers, but failed in clinical trials because of ineffectiveness and
greater side effects on the kidneys and heart. Some previous studies have confirmed that
simvastatin is a potential ABCB1 / P-gp inhibitor.
Statins are the most widely used anti-hypercholesterolemia in the world, through inhibition
of 3-hydroxy-3-methylglutaryl coenzyme-A reductase (Hmgcr) which is an enzyme that limits the
use of the mevalonate pathway that can be used as intracellular cholesterol. Besides having
pleiotropic effects, statins also have anti-tumor effects. At this time, statins have
received approval as a potential anti-tumor agent because several epidemiological studies
have agreed on the relationship between statin use and reducing the risk of recurrence of
LABC after adjuvant therapy. Some preclinical studies show that statins can decrease breast
cancer cell proliferation and induce apoptosis in various experimental models. results from
pre-operative "window-of-opportunity" clinical trials on LABC so that statins can reduce
tumor proliferation and induce apoptosis. Reports in the RSCM get simvastatin 40 mg for 4
weeks for neoadjuvant reduce the proliferation index in the LABC by 53.3% and inhibit the
increase in LABC cells through the Rho / Rock pathway. Although several studios of statin
antitumor activity have been carried out, the role of statins in oncology has not yielded
satisfactory results or controversies and provides heterogeneous responses depending on the
molecular identity and tumor type malignancy. The results of a clinical preliminary study
indicate that giving a single statin is not as effective as an anti-cancer because it
requires large effects and large side effects.
Several in vitro studies and animal models show that the combination of statins can increase
the accumulation of intra-cell chemotherapy so that the effects of potentiation of
chemotherapy arise. The administration of a combination of doxorubicin statins increases the
potential for anti-cancer effects through the accumulation of doxorubicin in cancer cells,
causing the potential for DNA damage, inhibition of proliferation, and induction of
apoptosis. statins can also protect cardiotoxic induced by doxorubicin if it is given
pre-therapy in mice. With a variety of anti-tumor mechanisms as well as the enormous benefits
and potential addition of statins that can be well-tolerated, safe, and inexpensive. However,
until now the effects of antiproliferation synergy and induction of apoptosis combination of
simvastatin and doxorubicin in LABC patients are not well known. This study aims to determine
the efficacy, tolerability, and safety of simvastatin combination and CAF chemotherapy as
neo-advanced therapy in LABC patients. The use of this combination is expected to improve
clinical and pathological responses as well as surgical margins while providing
cardioprotection effects, so as to provide the best service with high oncological value.
Methods
1. Subject and study design This research is a double-blind, placebo-controlled clinical
trial conducted at Dr. Cipto Mangunkusumo General Hospital and Koja General Hospital
from January 2018 to September 2019. Eligible patients are patients with grade IIIA to
IIIC invasive breast cancer that is histologically proven. A total of 60 LABC patients
were included in this study. Participants received a combination of NACT CAF and
Simvastatin (40 mg / day) (n = 30) or placebo (n = 30). Besides being used to make a
histopathological diagnosis, samples were taken by biopsy before NACT, examined for the
expression of HMG-CoA Reductase (HMGCR) and P-glycoprotein (P-gp). Participants were
evaluated for the clinical response after 3 NACT cycles. If it gives a complete or
partial response, then the patient will proceed to surgery. Then, the postoperative
specimen will be reviewed for a pathological response. However, if it is stable or
progressive, the patient will be given a 2nd line NACT.
2. Tumor assessment The primary outcome was clinical response while the secondary outcome
was the pathological response, incision boundary, P-gp expression, Hmgcr expression and
side effects. The analysis was performed on the population per protocol. Clinical
response assessment uses WHO 1979 criteria. Pathological responses of tumors are
evaluated according to the Miller-Payne scoring system. MPG classification is used to
evaluate the relevance between pathological response and clinical response. The incision
boundary assessment is performed using histopathological tissue incisions depending on
the surgical margins of the tumor on the medial, lateral, cranial, caudal, and baseline
sides of the tumor; based on the size of the new tumor. Histopathological results will
determine whether the level is free from the tumor or not based on the size of the new
tumor. Disease assessment is carried out by investigation after 3 NACT cycles. Side
effects were assessed during treatment and for 7 days after the last treatment dose and
assessed using CTCAE 3.0.
3. Biomarker assessment Estimation of P-glycoprotein (Pgp) and Hmgcr expression was seen
under a microscope from a sample after a core biopsy was performed before starting
chemotherapy. P-gp expression was interpreted based on the percentage of p-glycoprotein
positive cells in the total cell population (low = 0%, 1+ = 1-19%, and 2 + = 20-100%
positive cells). Hmgcr expression is interpreted based on the percentage of Hmgcr
positive cells in the total cell population (negative = 0%, 1+ = 1-10%, 2+ = 11-50%, 3+
=> 51-100% positive cells)..
4. Statistical analysis The main results in this study were clinical responses based on WHO
1970 criteria. ORR values in this study were calculated from the ratio of the number of
patients who showed a response (complete and partial) to the total number of patients
and were analyzed using the Pearson Chi-Square Test. Secondary outcomes in the form of
pathological responses based on GMP and incision boundaries were analyzed using Fisher's
Exact Test. Bivariate analysis of clinicopathological variables and molecular biology
with the therapeutic response using the Continuity Correction Test and the Fischer's
Exact Test. The results of the bivariate analysis with p> 0.25 were performed
multivariate analysis using the Logistic Regression Test. The analysis was performed
with the help of a computer using the SPSS 23 program. Differences were stated to be
meaningful and obtained p values <0.05.
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