Abstract 2110P
Background
Chemotherapy-induced nausea and vomiting (CINV) is the most common side effect following chemotherapy. For medium emetic chemotherapy (MEC), guidelines recommend dexamethasone (DEX) for the prevention and treatment of CINV. But the usage of DEX can cause a variety of adverse reactions. DEX-free regimens are being actively explored. Megestrol acetate (MA) was suggested as an antiemetic therapy gradually. Accordingly, the present phase II trial was designed to test the hypothesis that the efficacy of MA plus palonosetron regimen against CINV is non-inferior to a DEX regimen.
Methods
This was a randomized, self-controlled phase II study. Patients enrolled were scheduled to receive primary chemotherapy that contained oxaliplatin and fluorouracil every 3 weeks and randomized to the MA-DEX group or DEX-MA group. MA-DEX group received palonosetron (0.25 mg intravenously, d1) and MA (160 mg orally, d1-5)for first cycle and then received palonosetron and DEX (6 mg orally, d1-4) for second cycle. The DEX-MA group received the antiemetic treatment in the reverse order. The primary endpoint was complete response (CR). The non-inferiority margin was predefined as a 15% difference between groups in the primary endpoint. All subjects have signed the informed consent, and this trial has registered with Chinese Clinical Trial Register (ChiCTR2000037447).
Results
61 patients were eventually evaluated in the study 32 included in the DEX-MA group and 29 in the MA-DEX group. Overall CR rates were 82.25% for those administered MA on day 1 (acute phase) (n = 52), and 83.61% on days 2 -5 (delayed phase) (n = 51), 72.13% on days 1-7 (whole phase). According to CR rates,the MA regimen is non-inferior to DEX regimen during the acute, delayed and whole phase. Compared with DEX, the quality of life (QOL) of MA regimen was higher with respect to dyspnea (P=0.000) and appetite (P=0.021).
Conclusions
In this trial, MA is non-inferior to dexamethasone in the treatment of CINV induced by MEC regimens, and no obvious adverse reactions occurred. Compared with DEX, MA led to a milder dyspnea and appetite decrease, and better quality of life after chemotherapy.
Clinical trial identification
ChiCTR2000037447, 2020/08/27.
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
2085P - Buprenorphine use and cancer outcomes
Presenter: Nosayaba Osazuwa-Peters
Session: Poster session 06
2086P - Management of opioids use disorder in cancer survivors
Presenter: Khalida Berkane
Session: Poster session 06
2087P - Impact of cancer pain on quality of life and financial well-being: A cross-sectional study on symptom management
Presenter: Raffaele Giusti
Session: Poster session 06
2088P - Management of cancer treatment-induced bone loss in patients with breast and hormone sensitive prostate cancer: AIOM survey among Italian oncologists
Presenter: Anna Amela Valsecchi
Session: Poster session 06
2090P - Management of trastuzumab deruxtecan-related nausea and vomiting in real-world practice
Presenter: Luca Licata
Session: Poster session 06
2091P - Dermocosmetics in management of cancer-related skin toxicities: International expert consensus highlighting the key role of oncology nurses
Presenter: Pascale Dielenseger
Session: Poster session 06
2092P - Bone loss in premenopausal Algerian women treated with chemotherapy for early-stage of breast cancer: Evaluation by DXA and identification of associated risk factors
Presenter: MACHEROUM Fatma zohra
Session: Poster session 06
2093P - Bioelectrical Impedance phase angle and obesity as a prognostic indicator in metastatic gastric cancer patients receiving second-line chemotherapy
Presenter: SangUk Han
Session: Poster session 06
2094P - A multicenter phase II trial of the triplet antiemetic therapy with palonosetron, aprepitant and olanzapine for highly emetogenic chemotherapy in breast cancer
Presenter: Shinya Takada
Session: Poster session 06