Temozolomide and pasireotide treatment for aggressive pituitary adenoma: expertise at a tertiary care center

被引:0
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作者
Filippo Ceccato
Giuseppe Lombardi
Renzo Manara
Enzo Emanuelli
Luca Denaro
Laura Milanese
Marina Paola Gardiman
Roberta Bertorelle
Massimo Scanarini
Domenico D’Avella
Gianluca Occhi
Marco Boscaro
Vittorina Zagonel
Carla Scaroni
机构
[1] University-Hospital of Padova,Endocrinology Unit, Department of Medicine DIMED
[2] Veneto Institute of Oncology IOV - IRCCS,Department of Experimental and Clinical Oncology, Medical Oncology 1
[3] University of Salerno,Neuroradiology
[4] University-Hospital of Padova,Department of Otorhinolaryngology and Otologic Surgery
[5] University-Hospital of Padova,Neurosurgery, Department of Neurosciences DNS
[6] University-Hospital of Padova,Surgical Pathology and Cytopathology Unit, Department of Medicine DIMED
[7] Veneto Institute of Oncology IOV - IRCCS,Immunology and Molecular Oncology
[8] University-Hospital of Padova,Neurosurgical Division
[9] University of Padova,Department of Biology
来源
Journal of Neuro-Oncology | 2015年 / 122卷
关键词
Temozolomide; Pasireotide; Aggressive pituitary adenoma; Radiological shrinkage;
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学科分类号
摘要
Aggressive pituitary adenomas (PAs) are clinically challenging for endocrinologists and neurosurgeons due to their locally invasive nature and resistance to standard treatment (surgery, medical or radiotherapy). Two pituitary-directed drugs have recently been proposed: temozolomide (TMZ) for aggressive PA, and pasireotide for ACTH-secreting PA. We describe the experience of our multidisciplinary team of endocrinologists, neurosurgeons, neuroradiologists, oncologists, otolaryngologists and pathologists with TMZ and pasireotide treatment for aggressive PAs in terms of their radiological shrinkage and genetic features. We considered five patients with aggressive PA, three of them non-secreting (two ACTH-silent and one becoming ACTH secreting), and two secreting (one GH and one ACTH). TMZ was administrated orally at 150–200 mg/m2 daily for 5 days every 28 days to all 5 patients, and 2 of them also received pasireotide 600–900 µg bid sc. We assessed the MRI at the baseline and during TMZ or pasireotide treatment. We also checked for MGMT promoter methylation and IDH, BRAF and kRAS mutations. Considering TMZ, two patients showed PA progression, one stable disease and two achieved radiological and clinical response. Pasireotide was effective in reducing hypercortisolism and mass volume, combined with TMZ in one case. Both treatments were generally well tolerated; one patient developed a grade 2 TMZ-induced thrombocytopenia. None of patients developed hypopituitarism while taking TMZ or pasireotide treatment. No genetic anomalies were identified in the adenoma tissue. TMZ and pasireotide may be important therapies for aggressive PA, alone or in combination.
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页码:189 / 196
页数:7
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