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使用系列磁共振成像和肿瘤生长数学模型对低级别胶质瘤的侵袭性和增殖进行患者特异性表征。

Patient-specific characterization of the invasiveness and proliferation of low-grade gliomas using serial MR imaging and a mathematical model of tumor growth.

作者信息

Hathout Leith, Ellingson Benjamin M, Cloughesy Timothy F, Pope Whitney B

机构信息

Harvard Medical School, Boston, MA, USA.

Department of Radiological Sciences, David Geffen School of Medicine, University of California, Los Angeles, CA, USA.

出版信息

Oncol Rep. 2015 Jun;33(6):2883-8. doi: 10.3892/or.2015.3926. Epub 2015 Apr 27.

Abstract

Low-grade gliomas (LGGs) represent a significant proportion of hemispheric gliomas in adults. Although less aggressive than glioblastomas (GBMs), they have a broad range of biologic behavior, and often a limited prognosis. The aim of the present study was to explore LGG growth kinetics through a combination of routine MRI imaging and a novel adaptation of a mathematical tumor model. MRI imaging in 14 retrospectively identified grade II LGGs that showed some tumor enhancement was used to assess tumor radii at two separate time-points. This information was combined with a reaction-diffusion partial-differential equation model of tumor growth to calculate diffusion (D) and proliferation (ρ) coefficients for each tumor, representing measures of tumor invasiveness and cellular multiplication, respectively. The results were compared to previously published data on GBMs. The average value of D was 0.034 mm(2)/day and ρ was 0.0056/day. Grade II LGGs had a broad range of D and ρ. On average, the proliferation coefficient ρ was significantly lower than previously published values for GBM, by about an order of magnitude. The diffusion coefficient, modeling invasiveness, however, was only slightly lower but without statistical significance. It was possible to calculate detailed growth kinetic parameters for some LGGs, potentially providing a new way to assess tumor aggressiveness and possibly gauge prognosis. Even within a single-grade (WHO II), LGGs were found to have broad range of D and ρ, possibly correlating to their variable biologic behavior. Overall, the model parameters suggest that LGG is less aggressive than GBM based primarily on a lower index of tumor proliferation rather than on lesser invasiveness.

摘要

低级别胶质瘤(LGGs)在成人半球胶质瘤中占相当大的比例。尽管其侵袭性低于胶质母细胞瘤(GBMs),但其生物学行为范围广泛,且预后往往有限。本研究的目的是通过常规MRI成像与一种新型数学肿瘤模型相结合的方法来探索LGG的生长动力学。对14例经回顾性鉴定的II级LGGs进行MRI成像,这些肿瘤显示出一定程度的强化,用于在两个不同时间点评估肿瘤半径。该信息与肿瘤生长的反应扩散偏微分方程模型相结合,以计算每个肿瘤的扩散系数(D)和增殖系数(ρ),分别代表肿瘤侵袭性和细胞增殖的指标。将结果与先前发表的关于GBMs的数据进行比较。D的平均值为0.034 mm²/天,ρ为0.0056/天。II级LGGs的D和ρ范围广泛。平均而言,增殖系数ρ明显低于先前发表的GBM值,约低一个数量级。然而,模拟侵袭性的扩散系数仅略低,但无统计学意义。有可能为一些LGGs计算详细的生长动力学参数,这可能为评估肿瘤侵袭性和可能判断预后提供一种新方法。即使在单一级别(WHO II级)内,也发现LGGs的D和ρ范围广泛,这可能与其可变的生物学行为相关。总体而言,模型参数表明,LGG的侵袭性低于GBM,主要是基于较低的肿瘤增殖指数,而非较低的侵袭性。

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