Gastrointestinal Stromal Tumor Case Presentations

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Gastrointestinal Stromal Tumor Case Presentations Ricardo J. Gonzalez, MD Professor of Surgery Chair, Sarcoma Department Chief of Surgery Moffitt Cancer Center

Patient number 1 64 yo male with upper abdominal pain and palpable mass Biopsy consistent with C-KIT (+), DOG-1 (+) spindle cell neoplasm. CT Day 0 CT 12 mos Preop CT

Patient number 1 Exploratory laparotomy, resection of 4 th portion of duodenum and primary duodenojejunostomy

Phase II Trial of Neoadjuvant/Adjuvant Imatinib Mesylate (IM) for Advanced Primary and Metastatic/Recurrent Operable Gastrointestinal Stromal Tumor (GIST): Early Results of RTOG 0132/ACRIN 6665 N= 30 primary patients (Group A) N= 22 recurrent/metastatic patients (Group B) Patients with KITpositive, locally advanced (Group A [N=31]) or metastatic/ recurrent GIST (Group B [N=22]) Preoperative imatinib 600 mg/day x 8-12 wks SD/PR PD Resection Off study Imatinib 600 mg/day x 2 yrs Designed as a phase II feasibility trial for neoadjuvant imatinib given 8-12 weeks before planned surgery. Eisenberg J Surg Oncol 2009

Phase II Trial of Neoadjuvant/Adjuvant Imatinib Mesylate (IM) for Advanced Primary and Metastatic/Recurrent Operable Gastrointestinal Stromal Tumor (GIST): Early Results of RTOG 0132/ACRIN 6665 Failed Total 5-Yr Estimate All Patients 30 53 46.1% Primary 15 31 56.7% Recurrent/Mets 15 22 29.8% Med 8.9cm Size R0/R1 92% R2 8% 5.8cm 63% 32% Progression-Free Survival (%) Group A Group B 100 75 50 25 0 0 1 2 3 4 Yrs After Registration Concluded: Neoadjuvant imatinib is safe and feasible; requires multidisciplinary review and is not associated with post-op complications 5

Neoadjuvant therapy: when? May decrease the complexity of the procedure (adjacent organ involvement and tumor rupture/bleeding) 80% of patients benefit from imatinib, but CR s are very low Responses are frequent, yet metabolically inactive tumors harbor viable cells Surgery is planned usually within 9-12 months Demetri NEJM 2002 Antnescu Clin Can Res 2005 Verweij Lancet 2004

Metastasectomy and Debulking for Gastrointestinal Stromal Tumors

Patient number 2 86 yo male with right lower discomfort and fullness PET/CT time 0 PET/CT @ 30 days Preop CT at 6 mos

Patient number 2 Exploratory laparotomy, resection of jejunal GIST, and 2 peritoneal implants, no tumor rupture

Surgical Management of Advanced Gastrointestinal Stromal Tumors After Treatment With Targeted Systemic Therapy Using Kinase Inhibitors N=69 patients with advanced GIST (45 imatinib and 25 imatinib then sunitnib) Median f/u 14.6 months NED Min Residual Bulky Residual No % No % No % Total Stable disease 18 78 4 17.5 1 4.5 23 Limited progression 8 25 19 59 5 16 32 Generalized progression 1 7 7 50 6 43 14 Total 27 30 12 69 Raut JCO 2006

Surgical Management of Advanced Gastrointestinal Stromal Tumors After Treatment With Targeted Systemic Therapy Using Kinase Inhibitors Progression Free Survival R0/R1 Overall Survival 78% 7% 25% Concluded that patients with advanced or metastatic disease and stable or limited progression benefit from surgery Raut JCO 2006

Patient 3 70 yo male with a remote history of small bowel resection for a benign lesion. Upper abdominal pain CT imaging:

Treated to maximal Response Imatinib for 2 years Then referred to our Moffitt Cancer Center after progression noted Sunitinib started

Extended Right Hepatectomy Post-op 2 years later

Therapy by Type of Progression Limited or Nodular Progression Surgical Resection Hepatic Artery Chemoembolization Hepatic Radio-frequency Catheter Ablation Widespread progression Increase Imatinib to 800 mg daily Sunitinib Regorafenib Clinical Trial

Hepatic Artery Embolization Pre-embolization Post-embolization

Pre-embolization Post-embolization

Hepatic Arterial Embolization Radiographic Response Rates 14 patients with imatinib-resistant GIST and progressive liver metastases Treated with hepatic arterial embolization or chemoembolization 13 patients evaluable for radiologic response RESPONSE BEST RESPONSE (Choi Criteria) BEST RESPONSE (RECIST) Overall 54% 8% Complete 0% 0% Partial 54% 8% Stable 46% 92% Progression 0% 0% Kobayashi, K, et al. Am J Clin Oncol. 2009;32:574-581.

Hepatic Arterial Embolization Progression-Free Survival Kobayashi, K, et al. Am J Clin Oncol. 2009;32:574-581.

Regional Therapies for Sarcoma Jonathan Zager, MD Director of Regional Therapy

Hepatic Perfusion Started out as Isolated hepatic perfusion (IHP) in 1980 s and 1990 s at NCI Alexander, Bartlett and colleagues Supra Hepatic Cava Retro Hepatic Cava Portal Dissection/ Isolation Department of Cutaneous Oncology

Chemosaturation/PHP Isolation of Liver for Regional Tx Saturation of Liver with Melphalan Extracorporeal Filtration and Veno-Veno Bypass Department of Cutaneous Oncology

Department of Cutaneous Oncology Forster MF et al JSO 2013

Debulking Surgery Three retrospective studies have demonstrated a prolonged PFS in patients with response/stable disease and focal progression Surgery in metastatic GIST patients in the absence of MPD on imatinib is associated with outcomes at least comparable with second-line sunitinib and may be considered in select patients With generalized progression surgery may be considered for palliative intent Metastasectomy may enhance the effectiveness of TKI therapy in responders or stable disease

Gastrointestinal Stromal Tumor Case Presentations Ricardo J. Gonzalez, MD Professor of Surgery Chair, Sarcoma Department Chief of Surgery Moffitt Cancer Center

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