globalchange  > 影响、适应和脆弱性
项目编号: 1402739
项目名称:
kT-scale Protein & Carbohydrate Interactions on Synthetic Materials & Cell Surfaces
作者: Michael Bevan
承担单位: Johns Hopkins University
批准年: 2013
开始日期: 2014-06-01
结束日期: 2018-05-31
资助金额: USD308000
资助来源: US-NSF
项目类别: Standard Grant
国家: US
语种: 英语
特色学科分类: Engineering - Chemical, Bioengineering, Environmental, and Transport Systems
英文关键词: cell-cell ; cell migration ; cell-cell adhesion ; interaction ; other cellular process ; dcpm ; such interaction ; protein ; weak biological interaction ; stem-cell ; pi ; kt-scale protein ; cell surfaces many important cellular interaction ; weak biomolecular interaction ; heterophilic cadherin interaction ; tissue morphogenesis ; metastasis ; weak intermolecular interaction ; immunology ; carbohydrate interaction ; weak interaction ; cd44-ha interaction ; kt interaction ; strong interaction ; synthetic materials
英文摘要: PI: Bevan, Michael A.
Proposal Number: 1402739
Institution: Johns Hopkins University
Title: kT-scale Protein & Carbohydrate Interactions on Synthetic Materials & Cell Surfaces

Many important cellular interactions involve "weak" interactions, which are difficult to characterize by current techniques. The PI proposes to move into new territory, in terms of directly characterizing these weak intermolecular interactions of biomolecules, by using a technique, Diffusing Colloidal Probe Microscopy (DCPM), developed by the PI's group. The proposal will examine two systems of biological importance, which were also chosen for their significance to biomedical problems: stem-cell based tissue engineering and cancer metastasis. Success in the development of the technique for studying weak biological interactions will have an impact on the understanding of such interactions in cell-cell adhesion, cell migration, tissue morphogenesis, metastasis, immunology, and other cellular processes.

Weak biomolecular interactions, on the order of kT, play an important role in cell-cell adhesion, cell migration, tissue morphogenesis, metastasis, immunology, and other cellular processes. While there are standard mechanical methods for measuring strong interactions (>pN forces), weak interactions are generally measured_ indirectly_ by spectroscopic means. The PI proposes to move into new territory, by directly characterizing these interactions using DCPM, which offers spatial and temporal resolution, statistical significance, and directness not accessible using scanning probes or spectroscopic methods. In essence, DCPM passively monitors Brownian excursions of "diffusing probes" and exploits these natural gauges for time (a2/D), energy (kT), force (fN), and length (nm) when interrogating the interaction of proteins and carbohydrates. This is inherently a nanoscale technique because it harnesses Brownian motion as a useful tool to directly measure kT interactions between proteins rather than avoiding stochastic thermal motion as an undesirable complication of nanoscale systems. Two systems will be studied, CD44-HA interactions and heterophilic cadherin interactions (in the presence of calcium ions) on supported bilayers. The development of DCPM for studying weak biological interactions will have an impact on the understanding of such interactions in cell-cell adhesion, cell migration, tissue morphogenesis, metastasis, immunology, and other cellular processes.
资源类型: 项目
标识符: http://119.78.100.158/handle/2HF3EXSE/96830
Appears in Collections:影响、适应和脆弱性
气候减缓与适应

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Michael Bevan. kT-scale Protein & Carbohydrate Interactions on Synthetic Materials & Cell Surfaces. 2013-01-01.
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