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b'Patients eligible for inclusion in this study must meet all of the following criteria:' |
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b'Female sex' |
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b'Age \\u2265 18 and \\u2264 75 years.' |
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b'Evidence of a personally signed and dated informed consent document (ICD)' |
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b'indicating that the patient has been informed of all pertinent aspects of the' |
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b'tudy before enrollment' |
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b'Willingness and ability to comply with the prescribed FMD regimen, metformin' |
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b'intake, the scheduled visits, treatment plans, laboratory tests and other' |
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b'procedures.' |
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b'Histologically confirmed diagnosis of invasive TNBC candidate to neoadjuvant' |
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b'chemotherapy and subsequent curative surgery. On the basis of International' |
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b'Guidelines, TNBC is defined by absent or minimal (<1%) expression of oestrogen' |
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b'and progesterone receptors at IHC, and absence of HER2 over-expression or' |
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b'amplification, as defined as an IHC score of 0, 1+, or an IHC score of 2+ with in' |
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b'itu hybridization (ISH) analysis excluding HER2 gene amplification.' |
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b'Patients with localized disease (clinical stage I-III according to TNM). Patients' |
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b'with Stage I TNBC will be included only if the primary tumor is at least 10 mm in' |
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b'greatest dimension (clinical T1c as determined through baseline MRI assessment).' |
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b'Presence of an Eastern Cooperative Oncology Group (ECOG) performance status 0 or' |
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b'' |
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b'Presence of adequate bone marrow and organ function as defined by the following' |
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b'laboratory values:' |
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b'ANC \\u2265 1.5 x 103/l' |
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b'platelets \\u2265 100 x 103/l' |
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b'hemoglobin \\u2265 9.0 g/dl' |
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b'calcium (corrected for serum albumin) within normal limits or \\u2264 grade 1' |
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b'according to NCI-CTCAE version 5.0 if not clinically significant' |
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b'potassium within the normal limits, or corrected with supplements' |
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b'creatinine < 1.5 ULN' |
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b'blood uric acid < 10 mg/dl' |
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b'ALT and AST \\u2264 2 x ULN' |
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b'total bilirubin < 1.5 ULN except for patients with Gilbert syndrome who may' |
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b'only be included if the total bilirubin is < 3.0 x ULN or direct bilirubin <' |
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b'5 x ULN' |
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b'Fasting glucose \\u2264 250 mg/dl.' |
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b'Female patients of childbearing potential must agree to sexual abstinence or to' |
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b'use two highly effective methods of contraception throughout the study and for at' |
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b'least six months after the end of the FMD. Abstinence is only acceptable if it is' |
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b'in line with the preferred and usual lifestyle of the patient. Examples of' |
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b'contraceptive methods with a failure rate of < 1% per year include tubal' |
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b'ligation, male sterilization, hormonal implants, established, proper use of' |
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b'combined oral or injected hormonal contraceptives, and certain intrauterine' |
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b'devices. Alternatively, two methods (e.g., two barrier methods such as a condom' |
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b'and a cervical cap) may be combined to achieve a failure rate of < 1% per year.' |
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b'Barrier methods must always be supplemented with the use of a spermicide. A' |
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b'patient is of childbearing potential if, in the opinion of the Investigator, she' |
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b'is biologically capable of having children and is sexually active.' |
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b'Female patients are not of childbearing potential if they meet at least one of' |
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b'the following criteria:' |
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b'Have undergone a documented hysterectomy and/or bilateral oophorectomy' |
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b'Have medically confirmed ovarian failure' |
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b'Achieved post-menopausal status, defined as: \\u2265 12 months of' |
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b'non-therapy-induced amenorrhea or surgically sterile (absence of ovaries)' |
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b"and have a serum FSH level within the laboratory's reference range for" |
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b'postmenopausal females.' |
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b'Patients eligible for this study must not meet any of the following criteria:'
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b'Prior systemic treatment for breast cancer or other malignancies within 5 years'
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b'of treatment enrollment.'
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b'Prior treatment with anthracyclines'
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b'Diagnosis of other malignancies in advanced stages (unresectable, locally'
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b'advanced or metastatic), or that required systemic (neo)adjuvant chemotherapy in'
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b'the previous 5 years. Other malignancies diagnosed more than 5 years before the'
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b'diagnosis of breast cancer must have been radically treated without evidence of'
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b'relapse at the moment of patient enrollment in the trial.'
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b'Body mass index (BMI) < 20 kg/m2.'
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b'History of alcohol abuse.'
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b'Non-intentional weight loss \\u2265 5% in the previous 3 months, unless the patient has'
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b'a BMI > 22 kg/m2 and weight loss has been lower than 10% at the time of'
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b'enrollment in the study; or non-intentional weight loss of \\u2265 10% in the previous'
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b'3 months, unless the patients has a BMI > 25 kg/m2 and weight loss has been lower'
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b'than 15% at the time of the enrollment in the study. In both cases, weight must'
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b'have been stable for at least one month before study enrollment.'
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b'Active pregnancy or breast feeding.'
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b'Known active B or C hepatitis or human immunodeficiency virus (HIV) infection, or'
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b'occasional finding of active hepatitis B/C infection during screening tests'
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b'before chemotherapy initiation, as defined as positive polymerase chain reaction'
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b'(PCR) testing for HBV-DNA and HCV-RNA and qualitative PCR for HIV-RNA, or'
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b'requiring active treatment at study enrollment.'
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b'Serious infections in the previous 4 weeks before the FMD initiation, including,'
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b'but not limited to, potential hospitalizations for complications of infections,'
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b'bacteriemia or serious pneumonitis.'
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b'Active autoimmune diseases requiring systemic treatments (e.g. systemic steroids'
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b'or immune suppressants).'
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b'Active chronic therapy with systemic steroids at a dose \\u2265 10 mg per day of'
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b'prednisone or equivalent at study enrollment.'
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b'Known recent diagnosis of hypothyroidism requiring systemic replacement hormonal'
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b'therapy and without stabilization of hormonal profile (fT3, fT4 and TSH within'
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b'the normal range).'
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b'Diagnosis of type 1 or 2 diabetes mellitus requiring pharmacologic therapy'
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b'(including, but not limited to, insulin, secretagogues and metformin). A'
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b'diagnosis of type 2 diabetes mellitus not requiring pharmacological treatments'
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b'based on the judgment of a diabetologist, is compatible with patient enrollment'
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b'in the trial.'
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b'Active gastric or intestinal ulcerative disease, uncontrolled nausea, vomiting,'
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b'diarrhea, malabsorption syndrome, small intestine resection.'
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b'Anamnesis of clinically significant heart disease including:'
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b'angina pectoris, coronary bypass, symptomatic pericarditis, myocardial'
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b'infarction in the previous 12 months from the beginning of experimental'
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b'therapy;'
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b'congestive heart failure (NYHA III-IV).'
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b'Anamnesis of clinically meaningful cardiac arrhythmias, such as ventricular'
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b'tachycardia, chronic atrial fibrillation, complete bundle branch block, high'
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b'grade atrio-ventricular block like bi-fascicular block, type II Mobitz and third'
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b'grade atrio-ventricular block, nodal arrhythmias, supra-ventricular arrhythmia.'
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b'Left ventricular ejection fraction lower than 50% at the cardiac scan with'
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b'radionuclides or at echocardiography.'
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b'Previous episodes of symptomatic hypotension leading to loss of consciousness.'
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b'Baseline plasma fasting glucose \\u2264 60 mg/dL.'
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b'Medical or psychiatric comorbidities rendering the patient not candidate to the'
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b"clinical trial, according to the investigator's judgement."
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b'Other cardiac, liver, lung or renal comorbidities, not specified in the previous'
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b'risk of lactic acidosis.'
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