15 results on '"GIST - Gastrointestinal stromal tumor"'
Search Results
2. Managing endoscopic challenges on the road to resect a large ulcerated gastric GI stromal tumor
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Amrita Sethi, Kavel Visrodia, and Jorge Perales
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medicine.medical_specialty ,GiST ,business.industry ,ESE, endoscopic submucosal excavation ,digestive, oral, and skin physiology ,Gastroenterology ,GIST - Gastrointestinal stromal tumor ,social sciences ,Endoscopic submucosal dissection ,MP, muscularis propria ,GIST, gastrointestinal stromal tumor ,03 medical and health sciences ,0302 clinical medicine ,030220 oncology & carcinogenesis ,parasitic diseases ,ESD, endoscopic submucosal dissection ,population characteristics ,Medicine ,030211 gastroenterology & hepatology ,Radiology, Nuclear Medicine and imaging ,Radiology ,Stromal tumor ,Video Case Report ,business ,human activities - Abstract
Video Video 1 Managing endoscopic challenges on the road to resect a largeulcerated gastric GI stromal tumor.
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- 2021
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3. Endoscopic full-thickness resection of a stomach gastrointestinal stromal tumor using a dedicated full-thickness resection device
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Ashwini Esnakula, Yaseen B. Perbtani, Peter V. Draganov, Anand Gupte, and Dennis Yang
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SEL, subepithelial lesion ,medicine.medical_specialty ,GiST ,business.industry ,Full thickness resection device ,Stomach ,EFTR, endoscopic full thickness resection ,Gastroenterology ,GIST - Gastrointestinal stromal tumor ,GIST, gastrointestinal stromal tumor ,medicine.anatomical_structure ,Medicine ,Radiology, Nuclear Medicine and imaging ,Full thickness resection ,Radiology ,Stromal tumor ,Video Case Report ,business - Published
- 2020
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4. Advanced resection and closure techniques for endoscopic full-thickness resection in the gastric fundus
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Dmitriy O. Khodorskiy, Xiaocen Zhang, Stavros N. Stavropoulos, and Rani J. Modayil
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medicine.medical_specialty ,Gastric fundus ,GiST ,business.industry ,Gastroenterology ,Closure (topology) ,GIST - Gastrointestinal stromal tumor ,Surgery ,Resection ,GIST, gastrointestinal stromal tumor ,EFTR, endoscopic full-thickness resection ,Medicine ,Radiology, Nuclear Medicine and imaging ,Full thickness resection ,Video Case Report ,business ,SET, subepithelial tumor - Published
- 2020
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5. Disappearing pigmentary mosaicism during imatinib treatment for gastrointestinal stromal tumors
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Shawn E. Cowper, Jonathan S. Leventhal, Jill Lacy, Gauri Panse, and Emily Coleman
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Stromal cell ,GiST ,business.industry ,pigmentary mosaicism ,GIST - Gastrointestinal stromal tumor ,Case Report ,Imatinib ,Dermatology ,Imatinib treatment ,GIST, gastrointestinal stromal tumor ,gastrointestinal stromal tumors ,imatinib ,c-kit ,Cancer research ,Medicine ,business ,medicine.drug - Published
- 2019
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6. GIST: Correlation of risk classifications and outcome.
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Kersting S, Janot-Matuschek MS, Schnitzler C, Chourio Barboza DE, Uhl W, and Mittelkötter U
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- Humans, Mutation, Prognosis, Prospective Studies, Proto-Oncogene Proteins c-kit genetics, Receptor, Platelet-Derived Growth Factor alpha genetics, Retrospective Studies, Gastrointestinal Stromal Tumors diagnosis, Gastrointestinal Stromal Tumors pathology, Gastrointestinal Stromal Tumors surgery
- Abstract
In clinical practice, there are often discrepancies between the oncological prognosis of gastrointestinal stromal tumors (GIST) and the actual clinical course. This study aimed to check with our collective how reliably the current classifications (Miettinen, Fletcher) predict the prognosis of GIST and to evaluate whether an extension of the classifications by the parameter proliferation activity could make sense. This prospective study enrolled 58 patients who underwent surgery on GIST from 01/2006 to 12/2016. The postoperative course (curation, recurrence, progress) was correlated with the identified risk classification and the proliferative activity. Coincidences with other tumors were strikingly common in patients with GIST (43%). Based on the risk group assignment of GIST, no assessment of the probability of the occurrence of second neoplasia could be derived. Individual patients were under- or over-graduated concerning the assessment of biological behavior based on the standard risk classifications. The inclusion of proliferative activity did not allow for a more precise predictive power - neither to the risk of recurrence and metastasis nor to the development of a second neoplasia. The study showed that there is currently no parameter or logarithm that reliably predicts the biological behavior of GIST. Due to the frequency of coincidence of second neoplasia and (rare) distant metastases, for everyday clinical practice, appropriate staging diagnostic and regular follow-up care should also be used for benign GIST., Competing Interests: All authors completed the ICMJE uniform disclosure form. The authors have no conflicts of interest to declare., (©2022 JOURNAL of MEDICINE and LIFE.)
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- 2022
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7. Germline mutations in MSH2 and ATM gene in patients with GIST (gastrointestinal stromal tumor) and second epitelial tumors
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Giulia Venturi, Costanza Winchler, Francesca Gensini, Angelo Ferrara, Massimo Calistri, Francesca Castiglione, Michele Dimarino, Silvia Gasperoni, Enrico Mini, Caterina Bartoli, Martina Catalano, Antonio Taddei, Federico Perna, Roberta Giorgione, Lapo Bencini, Laura Papi, Fabio Cianchi, Luca Messerini, Filippo Nozzoli, and Roberta Sestini
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congenital, hereditary, and neonatal diseases and abnormalities ,Cancer Research ,business.industry ,GIST - Gastrointestinal stromal tumor ,Second primary cancer ,digestive system diseases ,Carney Triad ,Germline mutation ,Oncology ,Atm gene ,MSH2 ,Cancer research ,Medicine ,In patient ,business ,neoplasms - Abstract
e23520 Background: In adult GISTs are frequently sporadic, while rarely GISTs are linked to Carney Triad and Carney-Stratakis Syndrome and NF1. GISTs with second primary tumors are reported in 4-33% of patients in literature and genetic counseling is suggested to explore an underlying germline mutations pathway. Methods: In our Academic Hospital Centre (EURACAN member) in Florence, Italy, we are following patients with GIST and multiple primary tumors with genetic counseling (72 GISTs with second tumors/185 patients with GIST) and germline analysis of the following genetic panel is performed as clinically indicated: BRCA1, BRCA2, MUTYH, MLH1, MSH2, MSH6, CDH1, ATM, TP53, PTEN, CHECK2, PALB2, BARD1, BRIP1, BLM, RAD51C, RAD51D, XRCC2, PMS2, MRE11A, RAD50, NBN, FAM175A, EPKAM, TSK1, MEN1 by sequencing analysis with Illumina MiSeq by kit multiplicom BRCA Hereditary cancer Mastr plus, and bioinformatic analysis by software SOPHIADDM (Sophia genetics) for point genetic alterations of BRCA1 NM_007294.3, BRCA2 NM_000059.3, MUTYH NM_000249, MSH2 NM_000251, MSH6 NM_000179, CDH1 NM_00444360, ATM NM_000051, TP53 NM_000546, PTEN NM_000314, CHEK2 NM_001005735, PALB2 NM_024675, BARD1 NM_000465, BRIP1 NM_032043, BLM NM_000057, RAD51C NM_002876, RAD51D NM_001142571, XRCC2 NM_005431, PMS2 NM_000535, MRE11A NM_005590, RAD50 NM_006732, NBN NM_002485, FAM175A NM_139076, EPCAM NM_002354, STK1 NM_000455, MEN1 NM_000244 and MLPA (Multiplex Ligation-dependent Probe Amplification) test analysis for patients with kit P087-BRCA1,P045-BRCA2(CHEK2, P248-MLH1-MSH2, P003-MLH1/MSH2, P072-MSH6-MUTYH (MRC-Holland). Results: In 3 patients germline mutations have been observed: 1 patient showed the c.1192dupG, p.(Ala398Glyfs*19) pathogenic mutation in exon 7 of MSH2 gene, confirmed by Sanger Sequencing, 1 patient showed c.565-?_1130+?del mutation consisting in heterozygous 3-4-5-6 exons deletion of MSH2 gene, confirmed by MLPA analysis, and in 1 patient the following ATM alteration has been identified in heterozygosis: ATM c.5319+2T > C, p.(?). In the 2 patients with Lynch syndrome with colon adenocarcinoma (MSI-H), synchronous GISTs (1 patient quadruple WT and 1 patient kit ex 11 mutated ) were diagnosed; in the patient with ATM mutation, the diagnosis of GIST (kit ex 11 mutated) occurred after prostate adenocarcinoma and before colon adenocarcinoma (MSI-H). Conclusions: Our analysis suggests that GIST diagnosis could be tumor-related to multiple hereditary tumor syndromes as Lynch Syndrome and Ataxia-Teleangectasia syndrome, the latter being linked in eterozygosis to tumor susceptibility to breast in female. This report represents a high value in terms of genetic counseling for relatives and in terms of therapeutic implications for the patients.
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- 2021
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8. Update of NGS analysis of Italian survey of second tumors in patients with diagnosis of GIST (gastrointestinal stromal tumor)
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Margherita Nannini, Laura Papi, Giovanni Vancheri, Giovanni Grignani, Sara Manglaviti, Giovannella Palmieri, Alessandro Mazzocca, Giulia Meoni, Silvia Gasperoni, Angela Stefania Ribecco, Lorenzo Tofani, Francesca Castiglione, Margaret Ottaviano, Francesco Tolomeo, Agnese Paderi, Bruno Vincenzi, Tommaso Adragna, Elena Fumagalli, Enrico Mini, and Margherita Vannucchi
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Oncology ,Cancer Research ,medicine.medical_specialty ,GiST ,business.industry ,GIST - Gastrointestinal stromal tumor ,Second primary cancer ,digestive system diseases ,Internal medicine ,medicine ,In patient ,business ,neoplasms - Abstract
e23518 Background: In patients with GIST, literature reports a risk of second primary tumors between 4.5% and 33% with different distribution in the worldwide. The network of 7 italian EURACAN centers has collected clinical and molecular features of GIST patients with second primary tumors. Methods: We reviewed the clinical characteristics of 201 patients with GIST and second primary tumors in order to evaluate association between risk of dead and each possible factor, using Kaplan meier curve, log-rank test and Cox model for Hazard Ratio and it’s interval Confidence 95% estimation. Furthermore, NGS analysis ( 56 gene onco panel) in 72 patients with GIST was performed. Results: On the basis of the significant correlation previously observed between the Miettinen risk criteria of GIST (low/very low) and the incidence of second primary tumors (gastrointestinal tumors),P < 0.001 (Abstr 11032 ASCO 2019), we observed in these patients a median age of diagnosis of GIST of 68, with prevalent gastric site localization ( KIT exon 11 mutation), NF1 and Lynch (kit/pdgfra WT) syndromes in the low risk subgroup. The more frequent site of second epithelial tumor in gastrointestinal tract was the colon followed by gastric, pancreatic and biliary tract. In patients with GIST with low-very low risk according Miettinen classification, after a median follow-up period of 25 years, we have observed that the gastroenteric site of second tumors occurrence is significantly related to the survival (p < .0003). In the NGS analysis of the GIST we observed the pathogenetic somatic mutations in the following genes: BRCA 2 (p.Thr2125fs), but germline test negative, TP53 (p.Arg192*,p.Gly244Ser,p.His168Leu), RET (p.Lys120Asn, p.His168Leu, p.Thr930Met ), NRAS (p.Gly134Asp), CTNNB1 (p.Ser45Phe), MSH6 (P.Ala164Val), SMARCB1 (p.Arg192), VHL (p.Gly93Val), PTEN(p.Val158Ile, p.Asn323fs), STK1I (p.Arg40Cys), SMO (p.Glu194Lys), EGFR (p.Gly721Asp), ATM (p.Asp2708Asn), ERBB4 (p.Asn181Ile). Conclusions: In our analysis patients with GIST (low-very low classes according to Miettinen) have significant risk to death because of second primary tumors in gastrointestinal tract. Specific attention to gastrointestinal screening during the follow-up of GIST (low and very low risk) is required.
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- 2020
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9. Italian survey of second tumors in patients with diagnosis of GIST (gastrointestinal stromal tumor)
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Sara Fancelli, Lorenzo Tofani, Margaret Ottaviano, Maria Abbondanza Pantaleo, Giovannella Palmieri, Lorenzo D'Ambrosio, Lorena Incorvaia, Silvia Gasperoni, Giuseppe Badalamenti, Luca Messerini, Giovanni Grignani, Giulia Meoni, Margherita Nannini, Enrico Caliman, Agnese Paderi, Enrico Mini, Bruno Vincenzi, Elena Fumagalli, Sara Manglaviti, and Alessandro Mazzocca
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Cancer Research ,Pathology ,medicine.medical_specialty ,Oncology ,business.industry ,Mesenchymal stem cell ,medicine ,GIST - Gastrointestinal stromal tumor ,Digestive tract ,In patient ,business ,neoplasms ,digestive system diseases - Abstract
11032 Background: GISTs are the most common mesenchymal tumors of the digestive tract. As of recent, new links are being made between GISTS and secondary malignancies. However, whether the coexistence of GISTs with other tumors is stochastic, or the result of related pathogenetic mechanisms is still unknown. Methods: We retrospectively reviewed clinical and molecular features from all GIST patients with second tumors treated in seven Italian GIST reference centers. Qualitative variables were compared using the Fisher exact test. Results: Clinical data of 184 patients with diagnosis of GIST were evaluated. Median age at diagnosis was 66 years, KIT exon 11 resulted the most frequent mutation (73%) while seven patients (3.8%) had a genetic syndrome. The most common primary GIST localizations were stomach (54%) and small intestine (33%). Second tumors arose mostly from gastrointestinal and genitourinary tract. Fourtythree patients had two primary tumors other than GIST and five patients had three other primary malignancies. According to Miettinen criteria, 45% of non-metastatic patients at diagnosis belong to low or very low-risk classes. We highlighted a significant correlation (P=0.002) between risk class and second/third tumor localization, with considerably high percentage of GI second malignancies in low/very low risk GISTs (table). Conclusions: The high frequency of second/third tumors reported in low and very low GIST calls for a careful follow-up also in these patients. Furthermore, this population requires further genetic investigation, NGS analysis is ongoing. [Table: see text]
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- 2019
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10. Bowel Hot Spots at PET-CT
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Michael A. Blake, Dushyant V. Sahani, Peter R. Mueller, Alan J. Fischman, and Hima B. Prabhakar
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medicine.medical_specialty ,PET-CT ,medicine.diagnostic_test ,Practice patterns ,business.industry ,Fdg uptake ,GIST - Gastrointestinal stromal tumor ,Image Enhancement ,Intestinal Diseases ,Fluorodeoxyglucose F18 ,Positron emission tomography ,Positron-Emission Tomography ,Subtraction Technique ,Practice Guidelines as Topic ,medicine ,IBD - Inflammatory bowel disease ,Humans ,Radiology, Nuclear Medicine and imaging ,Radiology ,Tomography ,Practice Patterns, Physicians' ,Radiopharmaceuticals ,Tomography, X-Ray Computed ,business ,Nuclear medicine - Abstract
Positron emission tomography (PET) with 2-[fluorine-18]fluoro-2-deoxy-d-glucose (FDG) has been shown to be sensitive in the detection of many bowel malignancies, but its specificity is lower because of various physiologic and pathologic patterns of bowel FDG uptake. PET-computed tomography (CT) can be useful in localizing and characterizing foci of increased FDG uptake within the bowel. As the use of PET-CT in the staging and monitoring of oncologic disease continues to expand, familiarity with these patterns of bowel FDG uptake is essential and can help determine the need for and the relative urgency of further testing. Although a variety of imaging protocols are used for PET-CT, the use of negative oral contrast agent allows improved bowel distention while eliminating potential artifacts caused by high-density oral contrast agents. In addition, correlation with the CT portion of the combined PET-CT examination can sometimes help identify the cause of focal or segmental bowel uptake. The radiologist should be aware of potential pitfalls in the evaluation of FDG-avid foci within the abdomen, including bowel motility and low-attenuation lesions mimicking bowel. Nevertheless, even though the precise role of combined PET-CT for bowel assessment has yet to be determined, the application of sound basic principles of image interpretation will help ensure the accurate interpretation of bowel findings seen with this combined modality.
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- 2007
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11. A case of severe interstitial pneumonitis probably caused by imatinib mesylate in a patient with gastrointestinal stromal tumor
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Shigeto Oda, Yoshihisa Tateishi, Shin-ichi Sasagawa, Yasuhisa Abe, Hiroshi Sashiyama, Toshitaka Mamiya, and Hiroyuki Hirasawa
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Imatinib mesylate ,business.industry ,Cancer research ,GIST - Gastrointestinal stromal tumor ,Medicine ,Stromal tumor ,business ,Interstitial pneumonitis - Abstract
Gastrointestinal stromal tumor (GIST)の治療中に発生した,メシル酸イマチニブによると考えられる間質性肺炎を経験した。症例は82歳男性。消化管出血,腹腔内転移を伴うGISTに対し,メシル酸イマチニブの内服を開始し,原発巣,転移巣ともに著明な縮小を認めていた。内服開始35日目頃から労作時呼吸困難,咳嗽が出現し,38日目に入院した。胸部X線上広範囲のスリガラス状陰影を認め,急速に進行する高度の低酸素血症を示したため,同日人工呼吸管理とした。経過よりメシル酸イマチニブによる薬剤性間質性肺炎が疑われたため投与を中止し,メチルプレドニゾロン1g静注を3日間行ったところ,低酸素血症は改善した。その後,ステロイド内服下にメシル酸イマチニブを減量再開し,経過良好である。現時点でメシル酸イマチニブによる間質性肺炎の報告例は稀だが,使用に当たり十分な注意が必要と考えられた。
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- 2006
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12. GIST (gastrointestinal stromal tumor)
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Seiichi Hirota
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Oncology ,medicine.medical_specialty ,business.industry ,GIST - Gastrointestinal stromal tumor ,General Medicine ,Proto-Oncogene Proteins c-kit ,Text mining ,Internal medicine ,medicine ,Cancer research ,Humans ,business ,Gastrointestinal Neoplasms - Published
- 2004
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13. RADIOGRAPHIC CHARACTERISTICS OF GASTROINTESTINAL STROMAL TUMOR (GIST)
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Masaharu Miyazawa, Kazuo Kashiwazaki, Mamoru Watanabe, Hitoshi Ohtaka, Hidehiko Matsukawa, Nobuyuki Shiraga, Ehiichi Kohda, Hiromasa Ishii, Tokushige Oyama, Masao Kikuchi, Fumio Suzuki, and Toshifumi Hibi
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Leiomyosarcoma ,Cancer Research ,Gastrointestinal tract ,Pathology ,medicine.medical_specialty ,GiST ,business.industry ,Radiography ,CD34 ,GIST - Gastrointestinal stromal tumor ,medicine.disease ,Oncology ,medicine ,Immunohistochemistry ,Pharmacology (medical) ,Radiology ,Stromal tumor ,business - Published
- 2003
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14. Diagnostic et traitement des GIST (Gastrointestinal Stromal Tumor)
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Stephan Dirnhofer, C Knüsli, I Langer, Christoph Kettelhack, C Redaelli, M. Furrer, L Guillou, Markus Borner, Nicolas Demartines, Serge Leyvraz, U. Metzger, R. Burkhard, R von Moos, Luigi Tornillo, M von Flüe, and Michael Montemurro
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business.industry ,GIST - Gastrointestinal stromal tumor ,Cancer research ,Medicine ,business - Published
- 2008
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15. The GIST (Gastrointestinal Stromal Tumor) of the Gastroesophageal Junction (GEJ)
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Wanwarat Ananthapanyasut, Jue-lin Tang, Charles Berkelhammer, Andrea Blumenstein, and Sammy Nawas
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Pathology ,medicine.medical_specialty ,Hepatology ,business.industry ,Gastroenterology ,GIST - Gastrointestinal stromal tumor ,Medicine ,business ,Gastroesophageal Junction - Published
- 2007
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