Background & Aims
High-resolution microendoscopy is an optical imaging technique with the
potential to improve the accuracy of endoscopic screening for esophageal squamous
neoplasia. Although these microscopic images can readily be interpreted by trained
personnel, quantitative image analysis software could facilitate the use of this
technology in low-resource settings. In this study we developed and evaluated
quantitative image analysis criteria for the evaluation of neoplastic and non-neoplastic
squamous esophageal mucosa.
Methods
We performed image analysis of 177 patients undergoing standard upper endoscopy
for screening or surveillance of esophageal squamous neoplasia, using high-resolution
microendoscopy, at 2 hospitals in China and 1 in the United States from May 2010 to
October 2012. Biopsies were collected from imaged sites (n=375); a consensus diagnosis
was provided by 2 expert gastrointestinal pathologists and used as the standard.
Results
Quantitative information from the high-resolution images was used to develop an
algorithm to identify high-grade squamous dysplasia or invasive squamous cell cancer,
based on histopathology findings. Optimal performance was obtained using mean nuclear
area as the basis for classification, resulting in sensitivities and specificities of
93% and 92% in the training set, 87% and 97% in the test
set, and 84% and 95% in an independent validation set, respectively.
Conclusions
High-resolution microendoscopy with quantitative image analysis can aid in the
identification of esophageal squamous neoplasia. Use of software-based image guides may
overcome issues of training and expertise in low-resource settings, allowing for
widespread use of these optical biopsy technologies.
The risk of clinically-significant vitamin D deficiency increases at 25-hydroxyvitamin D levels below 20 ng/mL, according to the Institute of Medicine. By this standard, most cirrhotic hepatitis C virus (HCV)-positive patients and many non-cirrhotic patients are vitamin D deficient. The high prevalence of vitamin D deficiency among HCV patients is a cause for concern for several specific reasons. Classic studies established the importance of vitamin D and calcium in maintaining bone. Vitamin D's beneficial effects on bone are likely to be vital for HCV-infected patients because these individuals have a high prevalence of low bone mineral density. Many pharmaceutical agents reduce bone density and exposure to these drugs may increase bone disease in HCV-positive patients. Bone loss occurs following liver transplantation and bone density is often low in patients with HIV/HCV co-infection who are on combination antiretroviral therapy. Some evidence suggests that ribavirin reduces bone density, underscoring the special need to monitor vitamin D in patients receiving HCV treatment and to prescribe supplements, as appropriate. In addition to its role in calcium metabolism, vitamin D is also an immune modulator that reduces inflammation while enhancing protective immune responses. Higher vitamin D levels are associated with less liver fibrosis and less inflammation in HCV patients. Recent studies show that low vitamin D levels are associated with treatment failure among HCV-infected patients receiving pegylated-interferon and ribavirin. If confirmed, these findings will provide an additional reason to ensure adequate levels of vitamin D. The article concludes with information about how to monitor vitamin D status and how to use vitamin D supplements most effectively in HCV-infected patients.
There have been significant changes in operative strategy over time in the management of type A aortic dissection, with more frequent use of valve-sparing procedures, bioprosthetic aortic valve substitutes, antegrade cerebral perfusion strategies, and hypothermic circulatory arrest. Most importantly, a significant decrease of in-hospital mortality was observed during the 20-year timespan.
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