[1] This paper describes an algorithm for inferring cirrus cloud top and cloud base effective particle sizes and cloud optical thickness from the Moderate Resolution Imaging Spectroradiometer (MODIS) 0.645, 1.64 and 2.13, and 3.75 mm band reflectances/ radiances. This approach uses a successive minimization method based on a look-up library of precomputed reflectances/radiances from an adding-doubling radiative transfer program, subject to corrections for Rayleigh scattering at the 0.645 mm band, above-cloud water vapor absorption, and 3.75 mm thermal emission. The algorithmic accuracy and limitation of the retrieval method were investigated by synthetic retrievals subject to the instrument noise and the perturbation of input parameters. The retrieval algorithm was applied to three MODIS cirrus scenes over the Atmospheric Radiation Measurement Program's southern Great Plain site, north central China, and northeast Asia. The reliability of retrieved cloud optical thicknesses and mean effective particle sizes was evaluated by comparison with MODIS cloud products and qualitatively good correlations were obtained for all three cases, indicating that the performance of the vertical sizing algorithm is comparable with the MODIS retrieval program. Retrieved cloud top and cloud base ice crystal effective sizes were also compared with those derived from the collocated ground-based millimeter wavelength cloud radar for the first case and from the Cloud Profiling Radar onboard CloudSat for the other two cases. Differences between retrieved and radar-derived cloud properties are discussed in light of assumptions made in the collocation process and limitations in radar remote sensing characteristics.
The prevalence and clinical relevance of KIT mutations in childhood core-binding factor (CBF) acute myeloid leukemia (AML) have not been well characterized. In this study, a total of 212 children with de novo AML were enrolled from a Chinese population and 50 (23.5%) of the patients were deemed CBF-AML. KIT mutations were identified in 30% of the CBF-AML cohort. The KIT mutations were clustered in exon 17 and exon 8, and KIT mutations in exons 8 and 17 were correlated with a shorter overall survival (OS) (5-year OS: 30.0 ± 14.5% vs. 73.0 ± 8.5%, p = .007) and event-free survival (EFS) (5-year EFS: 30.0 ± 14.5% vs. 73.0 ± 8.5%, p = .003). Multivariate analysis revealed KIT mutations as an independent risk factor in CBF-AML. Our results suggest that KIT mutations are a molecular marker for an inferior prognosis in pediatric CBF-AML.
Previous studies have suggested an association between hepatitis C virus (HCV) infection and the development of Sjögren's syndrome (SS), also known as sicca syndrome. The main objective of this study was to summarize the existing evidence and quantitatively evaluate the association between hepatitis C virus infection and SS/sicca syndrome by performing a meta-analysis of observational studies. MEDLINE and PubMed (January 1980-August 2013) were searched to identify relevant studies in English. Outcomes were calculated and are reported as odds risk (OR) and 95% CIs based on a random-effects model. Heterogeneity was assessed with I 2 statistics. Quality assessment was performed with the Newcastle-Ottawa scale. Based on meta-analysis of five cross-sectional and five cohort studies, a significant positive relationship between HCV infection and development of SS/sicca syndrome was found, the pooled random effects OR being 3.31 (95% CI, 1.46-7.48; P < 0.001). In subset analyses, the studies that used European diagnostic criteria showed a higher summary OR than did studies that adopted other diagnostic criteria. When the data were stratified by source of controls, significant associations were also observed when healthy people (OR ¼ 9.44; 95% CI ¼ 2.67-33.40; P ¼ 0.204) or subjects with hepatitis B virus infection (OR ¼ 6.57; 95% CI ¼ 1.21-35.57; P ¼ 0.5) were used as controls, but not when the controls were hospital-based (OR ¼ 0.99; 95% CI ¼ 0.61-1.61; P ¼ 0.169). In summary, the findings suggest that HCV infection is associated with SS/sicca syndrome. The observed increased risk in studies in which European diagnostic criteria and healthy controls were used and the decreased risk in studies with hospital-based controls may be attributable to selection bias or other unknown factors.
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