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脊索瘤:病例系列及文献综述

Chordoma: a case series and review of the literature.

作者信息

Alan Ozkan, Akin Telli Tugba, Ercelep Ozlem, Tanrikulu Simsek Eda, Basoglu Tuylu Tugba, Mutis Aydan, Hasanov Rahib, Kaya Serap, Akgül Babacan Nalan, Dane Faysal, Yumuk Perran Fulden

机构信息

Division of Medical Oncology, Department of Internal Medicine, Marmara University Faculty of Medicine, Istanbul, Turkey.

Department of Internal Medicine, Marmara University Faculty of Medicine, Istanbul, Turkey.

出版信息

J Med Case Rep. 2018 Aug 27;12(1):239. doi: 10.1186/s13256-018-1784-y.

Abstract

BACKGROUND

Chordoma is a rare malignant tumor of the skull base and axial skeleton, with an incidence of less than 0.1/100,000 per year. Patients with advanced chordoma have a poor prognosis due to locoregional recurrence with infiltration and destruction of surrounding bone and soft tissue. Cytotoxic chemotherapy or other systemic therapies have not been proven to be effective for these diseases. Therefore, several molecularly targeted therapies have been proposed as potentially beneficial, including tyrosine kinase inhibitors such as imatinib, sorafenib, lapatinib, and others.

CASE PRESENTATION

We present three cases of advanced chordoma treated with molecular targeted therapies: a 52-year-old Caucasian man, a 72-year-old Caucasian woman, and a 38-year-old Caucasian woman.

CONCLUSIONS

Chordoma has few systemic treatment options and they have limited benefit. Randomized trials with large patient numbers are unfeasible in this rare disease. Targeted therapy might be a reasonable alternative treatment for chordoma. Still, new treatment strategies are needed for this rare disease.

摘要

背景

脊索瘤是一种罕见的颅底和中轴骨恶性肿瘤,年发病率低于十万分之一。晚期脊索瘤患者预后较差,因为局部区域会复发,并浸润和破坏周围骨骼及软组织。细胞毒性化疗或其他全身治疗方法尚未被证明对这些疾病有效。因此,已提出几种分子靶向治疗可能有益,包括酪氨酸激酶抑制剂,如伊马替尼、索拉非尼、拉帕替尼等。

病例报告

我们报告了三例接受分子靶向治疗的晚期脊索瘤病例:一名52岁的白人男性、一名72岁的白人女性和一名38岁的白人女性。

结论

脊索瘤的全身治疗选择很少,且益处有限。在这种罕见疾病中进行大规模患者的随机试验不可行。靶向治疗可能是脊索瘤合理的替代治疗方法。不过,这种罕见疾病仍需要新的治疗策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3967/6109974/a04cfb6fd8b3/13256_2018_1784_Fig1_HTML.jpg

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