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光子探测幼鼠脑组织和由于胎儿酒精中毒导致的分子特异性核纳米结构改变,采用光散射/定位方法。

Photonics probing of pup brain tissue and molecular-specific nuclear nanostructure alterations due to fetal alcoholism via light scattering/localization approaches.

机构信息

Mississippi State Univ., United States.

The Univ. of Tennessee Health Science Ctr., United States.

出版信息

J Biomed Opt. 2022 Jul;27(7). doi: 10.1117/1.JBO.27.7.076002.

Abstract

SIGNIFICANCE

Light is a good probe for studying the nanoscale-level structural or molecular-specific structural properties of brain cells/tissue due to stress, alcohol, or any other abnormalities. Chronic alcoholism during pregnancy, i.e., fetal alcoholism, being teratogenic, results in fetal alcohol syndrome, and other neurological disorders. Understanding the nano-to-submicron scale spatial structural properties of pup brain cells/tissues using light/photonic probes could provide a plethora of information in understanding the effects of fetal alcoholism.

AIM

Using both light scattering and light localization techniques to probe alterations in nano- to-submicron scale mass density or refractive index fluctuations in brain cells/tissues of mice pups, exposed to fetal alcoholism.

APPROACH

We use the mesoscopic physics-based dual spectroscopic imaging techniques, partial wave spectroscopy (PWS) and molecular-specific inverse participation ratio (IPR) using confocal imaging, to quantify structural alterations in brain tissues and chromatin/histone in brain cells, respectively, in 60 days postnatal mice pup brain, exposed to fetal alcoholism.

RESULTS

The finer focusing PWS analysis on tissues shows an increase in the degree of structural disorder strength in the pup brain tissues. Furthermore, results of the molecular-specific light localization IPR technique show an increase in the degree of spatial molecular mass density structural disorder in DNA and a decrease in the degree in histone.

CONCLUSIONS

In particular, we characterize the spatial pup brain structures from the molecular to tissue levels and address the plausible reasons for such as mass density fluctuations in fetal alcoholism.

摘要

意义

由于压力、酒精或其他任何异常情况,光可以很好地用于研究脑细胞/组织的纳米级结构或分子特异性结构特性。怀孕期间的慢性酒精中毒,即胎儿酒精中毒,具有致畸性,会导致胎儿酒精综合征和其他神经紊乱。使用光/光子探针了解幼鼠脑细胞/组织的纳米到亚微米级空间结构特性,可以提供大量信息,帮助了解胎儿酒精中毒的影响。

目的

使用光散射和光定位技术来探测暴露于胎儿酒精中毒的幼鼠脑细胞/组织中纳米到亚微米级质量密度或折射率波动的变化。

方法

我们使用基于介观物理的双光谱成像技术,部分波谱(PWS)和使用共焦成像的分子特异性反参与比(IPR),分别定量大脑组织和脑细胞中的染色质/组蛋白的结构变化,在暴露于胎儿酒精中毒的 60 天龄幼鼠大脑中。

结果

对组织进行更精细的聚焦 PWS 分析表明,幼鼠脑组织的结构无序强度增加。此外,分子特异性光定位 IPR 技术的结果表明,DNA 中空间分子质量密度结构无序程度增加,组蛋白中空间分子质量密度结构无序程度降低。

结论

特别是,我们从分子到组织水平表征了幼鼠大脑的结构,并探讨了胎儿酒精中毒中质量密度波动的可能原因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f601/9271689/3739026477a2/JBO-027-076002-g001.jpg

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