Fixed dose combination of capecitabine and cyclophosphamide in metastatic breast cancer: Results from THE ENCLOSE phase 2/3 randomized multicenter study.

Gupta, Sudeep; Biswas, Ghanashyam; Babu, Suresh; Maksud, Tanveer M; Lakshmaiah, Kuntegowdennahalli C; Patel, Jayanti G; Raja, Gopal; Boya, Rakesh R; Patil, Pramod; Choudhury, Kakali; Bondarde, Shailesh A; Neve, Rakesh S; Bhat, Guruprasad; Mamillapalli, Gopichand; Patel, Apurva A; Patel, Piyush; Joshi, Nisarg; Bajaj, Vinay; Khan, Mujtaba A

Gupta, Sudeep; Biswas, Ghanashyam; Babu, Suresh; Maksud, Tanveer M; Lakshmaiah, Kuntegowdennahalli C; Patel, Jayanti G; Raja, Gopal; Boya, Rakesh R; Patil, Pramod; Choudhury, Kakali; Bondarde, Shailesh A; Neve, Rakesh S; Bhat, Guruprasad; Mamillapalli, Gopichand; Patel, Apurva A; Patel, Piyush; Joshi, Nisarg; Bajaj, Vinay; Khan, Mujtaba A.

Afiliação

Gupta S; Tata Memorial Centre, Homi Bhabha National Institute, Mumbai, 400012, Maharashtra, India. Electronic address: sudeepgupta04@yahoo.com.
Biswas G; Sparsh Hospital and Critical Care Pvt. Ltd., Bhubaneshwar, 751007, Odisha, India.
Babu S; Life Care Hospital, Bangalore, 560029, Karnataka, India.
Maksud TM; Unique Hospital - Multispeciality & Research Institute, Surat, 395002, Gujarat, India.
Lakshmaiah KC; Srinivasam Cancer Care Hospitals India Pvt. Ltd., Bangalore, 560076, Karnataka, India.
Patel JG; Apple Hospital, Surat, 395002, Gujarat, India.
Raja G; Madras Medical College and Rajiv Gandhi Govt. General Hospital, Chennai, 600003, Tamil Nadu, India.
Boya RR; Mahatma Gandhi Cancer Hospital & Research Institute, Visakhapatnam, 530017, Andhra Pradesh, India.
Patil P; Kailash Cancer Hospital & Research Centre, Vadodara, 391760, Gujarat, India.
Choudhury K; Health Point Hospital, Kolkata, 700025, West Bengal, India.
Bondarde SA; Shatabdi Superspeciality Hospital, Nashik, 422005, Maharashtra, India.
Neve RS; P.D.E.A's Ayurved Rugnalay & Sterling Multispeciality Hospital, Pune, 411044, Maharashtra, India.
Bhat G; Mallikatta Neuro Centre, Mangalore, 575003, Karnataka, India.
Mamillapalli G; City Cancer Centre, Vijayawada, 520002, Andhra Pradesh, India.
Patel AA; The Gujarat Cancer & Research Institute (M.P. Shah Cancer Hospital), Ahmedabad, 380016, Gujarat, India.
Patel P; Medical Affairs and Clinical Development, Intas Pharmaceuticals Ltd., Ahmedabad, 380054, Gujarat, India.
Joshi N; Medical Affairs and Clinical Development, Intas Pharmaceuticals Ltd., Ahmedabad, 380054, Gujarat, India.
Bajaj V; Medical Affairs and Clinical Development, Intas Pharmaceuticals Ltd., Ahmedabad, 380054, Gujarat, India.
Khan MA; Medical Affairs and Clinical Development, Intas Pharmaceuticals Ltd., Ahmedabad, 380054, Gujarat, India.

Breast ; 60: 147-154, 2021 Dec.

Article em En | MEDLINE | ID: mdl-34624757

ABSTRACT

ABSTRACT

AIM:

To evaluate pharmacokinetics, efficacy and safety of fixed-dose combination (FDC) of oral capecitabine + cyclophosphamide in metastatic breast cancer (MBC) patients progressing after anthracycline and/or taxane chemotherapy.

METHODS:

In this prospective, adaptive, phase-2/3, open-label study (CTRI/2014/12/005234), patients were randomized (111) to three FDC doses (doses/day D1, capecitabine + cyclophosphamide 1400 mg + 60 mg; D2, 1800 mg + 80 mg; D3, 2200 mg + 100 mg) for 14 days, in 21-day cycles. In Part-I, multiple-dose pharmacokinetics and optimal dose(s) were evaluated with futility analysis. Group(s) with <3 responders based on best overall response rate (BOR, complete response [CR]+partial response [PR]), were discontinued. Efficacy (BOR, disease control rates [DCR; CR + PR + stable disease]) and safety of optimal dose(s) were evaluated in Part-II.

RESULTS:

Of 66 patients (n = 22/group) in Part-I, pharmacokinetics (D1 = 7/22, D2 = 9/22, D3 = 8/22) showed dose-proportionality for cyclophosphamide and greater than dose-proportionality for capecitabine. Modified intent-to-treat (mITT) analysis showed BOR of 7.14% (1/14) in D1 (discontinued), and 22.22% (4/18) each in D2 and D3, respectively. In Part-II, 50 additional patients were randomized in D2 and D3 (n = 144; total 72 [22 + 50] patients/group). mITT analysis in D2 (n = 54) and D3 (n = 58) showed BOR of 29.63% (16/54, 95%CI 17.45-41.81%) and 22.41% (13/58, 95%CI 11.68-33.15%), respectively. DCR in D2 and D3 were 87.04% (47/54, 95%CI 78.08-96.00%) and 82.76% (48/58; 95%CI 73.04-92.48%) after 3 and 57.41% (31/54; 95%CI 52.41-79.50%) and 50.00% (29/58; 95%CI 40.40-67.00%), after 6-cycles, respectively. Hand-foot syndrome (16.67%), vomiting (9.72%) in D2, and hand-foot syndrome (18.06%), asthenia (15.28%) in D3 were most-common adverse events.

CONCLUSION:

FDC of capecitabine + cyclophosphamide (1800 + 80 mg/day) showed high disease control rates and good safety profile in MBC patients.

Assuntos

Neoplasias da Mama; Protocolos de Quimioterapia Combinada Antineoplásica/efeitos adversos; Neoplasias da Mama/tratamento farmacológico; Capecitabina/uso terapêutico; Ciclofosfamida/efeitos adversos; Desoxicitidina/efeitos adversos; Feminino; Fluoruracila/uso terapêutico; Humanos; Metástase Neoplásica; Estudos Prospectivos; Resultado do Tratamento

Palavras-chave

Capecitabine; Cyclophosphamide; FDC; Fixed-dose combination; MBC

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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Neoplasias da Mama Tipo de estudo: Clinical_trials / Observational_studies / Risk_factors_studies Limite: Female / Humans Idioma: En Revista: Breast Assunto da revista: ENDOCRINOLOGIA / NEOPLASIAS Ano de publicação: 2021 Tipo de documento: Article

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