کد مقاله | کد نشریه | سال انتشار | مقاله انگلیسی | نسخه تمام متن |
---|---|---|---|---|
8038275 | 1518332 | 2014 | 16 صفحه PDF | دانلود رایگان |
عنوان انگلیسی مقاله ISI
Multimodal nanoparticles as alignment and correlation markers in fluorescence/soft X-ray cryo-microscopy/tomography of nucleoplasmic reticulum and apoptosis in mammalian cells
ترجمه فارسی عنوان
نانوذرات چندجملهای به عنوان همبستگی و نشانگرهای همبستگی در کریو میکروسکوپی / اشعه ماوراء بنفش اشعه ایکس / فلورسانس سلول های خونی و آپوپتوز در سلول های پستانداران
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کلمات کلیدی
PAHPSSeGFPNECn.a.X-ray imaging - تصویربرداری با اشعه ایکسLive-cell imaging - تصویربرداری سلول زندهnumerical aperture - دیافراگم عددیNucleoplasmic reticulum - شبکیه نوکلئوپلاسمیکGold nanoparticles - نانوذرات طلاquantum dots - نقاط کوانتومیenhanced green fluorescent protein - پروتئین فلورسنت سبز افزایش یافته استPoly(styrene sulfonate) - پلی استایرن سولفوناتpoly(allylamine hydrochloride) - پلی هیدروکلراید (آللیامین)
موضوعات مرتبط
مهندسی و علوم پایه
مهندسی مواد
فناوری نانو (نانو تکنولوژی)
چکیده انگلیسی
Correlative fluorescence and soft X-ray cryo-microscopy/tomography on flat sample holders is perfectly suited to study the uncompromised physiological status of adherent cells at its best possible preservation by imaging after fast cryo-immobilization. To understand the mechanism by which herpesviruses induce nucleoplasmic reticulum, i.e. invaginations of the nuclear envelope, during their egress from the host cell nucleus, morphologically similar structures found in laminopathies and after chemical induction were investigated as a potentially more easily accessible model system. For example, anti-retroviral protease inhibitors like Saquinavir also induce invaginations of the nuclear membranes. With the help of newly designed multimodal nanoparticles as alignment and correlation markers, and by optimizing fluorescence cryo-microscopy data acquisition, an elaborate three-dimensional network of nucleoplasmic reticulum was demonstrated in nuclei of Saquinavir-treated rabbit kidney cells expressing a fluorescently labeled inner nuclear membrane protein. In part of the protease inhibitor-treated samples, nuclei exhibited dramatic ultrastructural changes indicative of programmed cell death/apoptosis. This unexpected observation highlights another unique feature of soft X-ray microscopy, i.e. high absorption contrast information not relying on labeled cellular components, at a 3D resolution of approximately 40Â nm (half-pitch) and through a sample thickness of several micrometers. These properties make it a valuable part of the cell biology imaging toolbox to visualize the cellular ultrastructure in its completeness.
ناشر
Database: Elsevier - ScienceDirect (ساینس دایرکت)
Journal: Ultramicroscopy - Volume 146, November 2014, Pages 46-54
Journal: Ultramicroscopy - Volume 146, November 2014, Pages 46-54
نویسندگان
Christoph Hagen, Stephan Werner, Susana Carregal-Romero, Ashraf N. Malhas, Barbara G. Klupp, Peter Guttmann, Stefan Rehbein, Katja Henzler, Thomas C. Mettenleiter, David J. Vaux, Wolfgang J. Parak, Gerd Schneider, Kay Grünewald,