首页> 外文期刊>The Analyst: The Analytical Journal of the Royal Society of Chemistry: A Monthly International Publication Dealing with All Branches of Analytical Chemistry >Native fluorescence spectroscopic characterization of DMBA induced carcinogenesis in mice skin for the early detection of tissue transformation
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Native fluorescence spectroscopic characterization of DMBA induced carcinogenesis in mice skin for the early detection of tissue transformation

机译:DMBA诱导小鼠皮肤癌变的天然荧光光谱表征,可早期检测组织转化

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摘要

The objective of the study is to characterize the endogenous porphyrin fluorescence in a dimethylbenz(a)anthracene (DMBA) induced mouse skin tumor model using native fluorescence emission and excitation spectroscopy. Two intensity ratio parameters I580/I635 and I420/I515 were selected to represent the key fluorophore of endogenous porphyrins from emission and excitation spectra recorded in vivo from 31 DMBA treated animals and 5 control animals. In the emission spectrum, the endogenous porphyrin was elevated at 635 nm in different transformation lesions such as hyperplasia, papilloma, dysplasia, ESCC and WDSCC. This is corroborated by the endogenous porphyrin elevation at 420, 515, 550 and 588 nm in the WDSCC lesions from the excitation spectra. The elevation of endogenous porphyrin, probably protoporphyrin IX (PpIX), is due to biochemical and metabolic alterations in epithelial cells during tissue transformation. The loss of ferrochelatase activity might be responsible for enhanced PpIX in the transformed tissues. The sensitivity and specificity were determined for different lesion pairs from the scatter plot based on the discrimination value by validation with histopathological results. The emission intensity ratio I580/I635 at 405 nm excitation was selected to discriminate normal from hyperplasia, hyperplasia from papilloma, papilloma from dysplasia, dysplasia from early squamous cell carcinoma (ESCC), and ESCC from well differentiated squamous cell carcinoma (WDSCC) with specificities of 100%, 88%, 100%, 86%, and 100% and sensitivities of 100%, 80%, 100%, 100% and 100% respectively. Similarly, the excitation intensity ratio I420/I515 for 635 nm emission used to discriminate between WDSCC lesions and normal tissue gives 100% specificity and 100% sensitivity.
机译:该研究的目的是使用天然荧光发射和激发光谱法在二甲基苯并蒽(DMBA)诱导的小鼠皮肤肿瘤模型中表征内源性卟啉荧光。从31只DMBA处理的动物和5只对照动物体内记录的发射和激发光谱中,选择两个强度比参数I580 / I635和I420 / I515代表内源卟啉的关键荧光团。在发射光谱中,内源性卟啉在增生,乳头状瘤,不典型增生,ESCC和WDSCC等不同转化病变中在635 nm处升高。 WDSCC病变中的内源性卟啉在420、515、550和588 nm处的激发光谱证实了这一点。内源性卟啉(可能是原卟啉IX(PpIX))的升高是由于组织转化过程中上皮细胞的生化和代谢改变。铁螯合酶活性的丧失可能是导致转化组织中PpIX增强的原因。通过与组织病理学结果的验证,基于辨别值从散点图中确定不同病变对的敏感性和特异性。选择在405 nm激发下的发射强度比I580 / I635以正常区分增生,乳头状瘤增生,发育不良的乳头状瘤,早期鳞状细胞癌(ESCC)的发育异常和高分化鳞状细胞癌(WDSCC)的ESCC具有特异性分别为100%,88%,100%,86%和100%,灵敏度分别为100%,80%,100%,100%和100%。类似地,用于区分WDSCC病变和正常组织的635 nm发射的激发强度比I420 / I515给出了100%的特异性和100%的灵敏度。

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