The morphology study shows the blisters formation on the Kapton polymer surface due to 1.25 MeV gamma rays irradiation at ambient temperature. This observation PHA-848125 provides a basis for the quantitative evaluation of FTIR results obtained for thermally stable polymer on the chemical bond deterioration with increasing gamma irradiation. The blistering mechanism is correlated with the internal gases (CO, H(2)) released due to gamma radiation induced damages. The recorded UV-VIS spectrum shows a maximum absorption around the wavelength 540 nm. However, the nature of the spectra does not change due to gamma irradiation but

a shift in absorption edge towards the higher wavelength side has been observed with increasing dose. The optical data shows an increase in the calculated band gap at the highest dose. The diffraction pattern of virgin sample shows that polymer is semicrystalline, but due to irradiation, a decrease in the peak intensity and FWHM and an increase in the crystallite size at the highest dose level of 300 kGy have been observed. (C) 2011 Wiley Periodicals, Inc. J Appl Polym Sci 120: 2928-2937, 2011″
“PURPOSE: To evaluate the repeatability of Fourier-domain optical coherence tomography (OCT) pachymetric mapping and compare central corneal thickness (CCT) measurements

by OCT, ultrasound pachymetry, and scanning-slit tomography.

SETTING: Doheny Eye Institute, University of Southern California, Los Angeles, California, USA.

METHODS: A Fourier-domain OCT system was used to map the corneal Mocetinostat clinical trial thickness in normal eyes with scans centered on the corneal vertex or the pupil. Repeatability of central and pericentral map sectors was assessed by pooled standard deviation. The CCT measurements were compared between the OCT, ultrasound, and scanning-slit devices.

RESULTS: Pupil centration (SD: 1.3 mu m central, 1.8 to 3.8 mu m pericentral) provided better repeatability than vertex centration (SD: 1.7 mu m central, 2.4 to 5.7 mu m pericentral) in all sectors (P<.035). The mean CCT was 536.9 mu m +/- 27.0 MEK inhibitor (SD) by OCT, 556.6 +/- 30.5 mu

m by ultrasound, and 537.2 +/- 32.6 mu m by scanning-slit tomography (acoustic factor 0.92). The CCT measured by OCT was significantly thinner than by ultrasound pachymetry (P = .007; mean difference -19.7 mu m; 95% limits of agreement [LoA], -40.4 to 0.9 mu m) but not than by scanning-slit tomography (P = .2637; mean difference -0.3 mu m; 95% LoA, -24.0 to 23.5 mu m). The CCT by OCT correlated well with ultrasound and scanning-slit CCTs (r = 0.940 and r = 0.934, respectively).

CONCLUSION: Pachymetric mapping with Fourier-domain OCT was highly repeatable. Repeatability was better with pupil-centered scans than with corneal vertex centered scans. Ultrasound pachymetry, Fourier-domain OCT, and scanning-slit tomography should not be used interchangeably for CCT assessment.