106 research outputs found
p53 as a biomarker and potential target in gastrointestinal stromal tumors
KIT and PDGFRA play a major role in the oncogenic process in gastrointestinal stroma tumors (GIST) and small molecules have been employed with great success to target the KIT and PDGFRA pathways in this cancer. However, approximately 10% of patients with GIST are resistant to current targeted drug therapy. There is a need to explore other potential targets. Although p53 alterations frequently occur in most cancers, studies regarding p53 in GIST have been limited. The CDKN2A/MDM2/p53 axis regulates cell cycle progression and DNA damage responses, which in turn control tumor growth. This axis is the major event required for transformation from low- to high-risk GIST. Generally, p53 mutation is infrequent in GIST, but p53 overexpression has been reported to be associated with high-risk GIST and unfavorable prognosis, implying that p53 should play a critical role in GIST. Also, Wee1 regulates the cell cycle and the antitumor activity of Wee1 inhibition was reported to be p53 mutant dependent. In addition, Wee1 was reported to have potential activity in GIST through the regulation of KIT protein and this mechanism may be dependent on p53 status. In this article, we review previous reports regarding the role of p53 in GIST and propose targeting the p53 pathway as a novel additional treatment strategy for GIST
MEMO: Dataset and Methods for Robust Multimodal Retinal Image Registration with Large or Small Vessel Density Differences
The measurement of retinal blood flow (RBF) in capillaries can provide a
powerful biomarker for the early diagnosis and treatment of ocular diseases.
However, no single modality can determine capillary flowrates with high
precision. Combining erythrocyte-mediated angiography (EMA) with optical
coherence tomography angiography (OCTA) has the potential to achieve this goal,
as EMA can measure the absolute 2D RBF of retinal microvasculature and OCTA can
provide the 3D structural images of capillaries. However, multimodal retinal
image registration between these two modalities remains largely unexplored. To
fill this gap, we establish MEMO, the first public multimodal EMA and OCTA
retinal image dataset. A unique challenge in multimodal retinal image
registration between these modalities is the relatively large difference in
vessel density (VD). To address this challenge, we propose a segmentation-based
deep-learning framework (VDD-Reg) and a new evaluation metric (MSD), which
provide robust results despite differences in vessel density. VDD-Reg consists
of a vessel segmentation module and a registration module. To train the vessel
segmentation module, we further designed a two-stage semi-supervised learning
framework (LVD-Seg) combining supervised and unsupervised losses. We
demonstrate that VDD-Reg outperforms baseline methods quantitatively and
qualitatively for cases of both small VD differences (using the CF-FA dataset)
and large VD differences (using our MEMO dataset). Moreover, VDD-Reg requires
as few as three annotated vessel segmentation masks to maintain its accuracy,
demonstrating its feasibility.Comment: Submitted to IEEE JBH
A Genetic Polymorphism (rs17251221) in the Calcium-Sensing Receptor Gene (CASR) Is Associated with Stone Multiplicity in Calcium Nephrolithiasis
Calcium nephrolithiasis is one of the most common causes of renal stones. While the prevalence of this disease has increased steadily over the last 3 decades, its pathogenesis is still unclear. Previous studies have indicated that a genetic polymorphism (rs17251221) in the calcium-sensing receptor gene (CASR) is associated with the total serum calcium levels. In this study, we collected DNA samples from 480 Taiwanese subjects (189 calcium nephrolithiasis patients and 291 controls) for genotyping the CASR gene. Our results indicated no significant association between the CASR polymorphism (rs17251221) and the susceptibility of calcium nephrolithiasis. However, we found a significant association between rs17251221 and stone multiplicity. The risk of stone multiplicity was higher in patients with the GG+GA genotype than in those with the AA genotype (chi-square test:P = 0.008;odds ratio  =  4.79;95% confidence interval, 1.44–15.92;Yates' correction for chi-square test:P = 0.013). In conclusion, our results provide evidence supporting the genetic effects of CASR on the pathogenesis of calcium nephrolithiasis
Blockwise-Lattice-Reduction Aided Precoders for Multiuser MIMO with Clusters of Correlated Users
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