- About
-
The Global ETD Search service is a free service for researchers
to find electronic theses and dissertations. This service is
provided by the
Networked Digital Library of Theses and Dissertations.
Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
Search results
Showing 161 to 170 of 569 (0.035 seconds)Spelling suggestions: "subject:"[een] TRACTION"" "subject:"[enn] TRACTION""
| 161 |
熱変形分布を規定する熱弾性場における形状同定問題の解法片峯, 英次, KATAMINE, Eiji, 平井, 雅大, HIRAI, Masahiro, 畔上, 秀幸, AZEGAMI, Hideyuki 09 1900 (has links)
No description available.
|
| 162 |
力法を用いた有限要素モデルのモーフィング笹岡, 竜, Sasaoka, Ryu, 足達, 一真, Adachi, Kazuma, 畔上, 秀幸, Azegami, Hideyuki 11 1900 (has links)
No description available.
|
| 163 |
対流項を考慮した粘性流れ場の形状最適化問題の解法片峯, 英次, KATAMINE, Eiji, 津幡, 知幸, TSUBATA, Tomoyuki, 畔上, 秀幸, AZEGAMI, Hideyuki 11 1900 (has links)
No description available.
|
| 164 |
形状最適化問題の解法における多制約の取り扱い小山, 悟史, KOYAMA, Satoshi, 畔上, 秀幸, AZEGAMI, Hideyuki 10 1900 (has links)
No description available.
|
| 165 |
Solution to Shape Optimization Problem of Linear Elastic Continuum with Prescribed Vibrational Eigen-modeINZARULFAISHAM, Abd Rahim, AZEGAMI, Hideyuki 03 1900 (has links)
Proceedings of the 50th JSME Tokai Branch Meeting. n.013-1, 2001, p.97-98
|
| 166 |
規定した変形を生む異種材料境界面の形状設計畔上, 秀幸, AZEGAMI, Hideyuki, 小山, 悟史, KOYAMA, Satoshi 11 1900 (has links)
No description available.
|
| 167 |
脊柱有限要素モデルの個体別モデリング笹岡, 竜, Sasaoka, Ryu, 畔上, 秀幸, AZEGAMI, Hideyuki 01 1900 (has links)
No description available.
|
| 168 |
Hybrid methods for inverse force estimation in structural dynamicsSehlstedt, Niklas January 2003 (has links)
No description available.
|
| 169 |
Vorderasiatische Wagentypen : im Spiegel der Terracottaplastik bis zur altbabylonischen Zeit /Bollweg, Jutta. January 1900 (has links)
Dissertation--Universität Bern, 1996. / Bref résumé en anglais. Bibliogr. p. 60-72.
|
| 170 |
Regulation of Cell Adhesion Strength by Spatial Organization of Focal AdhesionsElineni, Kranthi Kumar 01 January 2011 (has links)
Cell adhesion to extracellular matrix (ECM) is critical to various cellular processes like cell spreading, migration, growth and apoptosis. At the tissue level, cell adhesion is important in the pathological and physiological processes that regulate the tissue morphogenesis. Cell adhesion to the ECM is primarily mediated by the integrin family of receptors. The receptors that are recruited to the surface are reinforced by structural and signaling proteins at the adhesive sites forming focal adhesions that connect the cytoskeleton to further stabilize the adhesions. The functional roles of these focal adhesions extend beyond stabilizing adhesions and transduce mechanical signals at the cell-ECM interface in various signaling events. The objective of this research is to analyze the role of the spatial distribution of the focal adhesions in stabilizing the cell adhesion to the ECM in relation to cell's internal force balance. The central hypothesis was that peripheral focal adhesions stabilize cell adhesion to ECM by providing for maximum mechanical advantage for resisting detachment as explained by the membrane peeling mechanism. Micropatterning techniques combined with robust hydrodynamic shear assay were employed to test our hypothesis. However, technical difficulties in microcontact printing stamps with small and sparse features made it challenging to analyze the role of peripheral focal adhesions in stabilizing cell adhesion. To overcome this limitation, the roof collapse phenomenon in stamps with small and sparse features (low fill factor stamps) that was detrimental to the reproduction of the adhesive geometries required to test the hypothesis was analyzed. This analysis lead to the valuable insight that the non-uniform pressure distribution during initial contact caused by parallelism error during manual microcontact printing prevented accurate replication of features on the substrate. To this end, the template of the stamp was modified so that it included an annular column around the pattern zone that acted as a collapse barrier and prevented roof collapse propagation into the pattern zone. Employing this modified stamp, the required geometries for the cell adhesion analysis were successfully reproduced on the substrates with high throughput. Adhesive areas were engineered with circular and annular patterns to discern the contribution of peripheral focal adhesions towards cell adhesion strength. The patterns were engineered such that two distinct geometries with either constant adhesive area or constant spreading area were obtained. The significance of annular patterns is that for the same total adhesive area as the circular pattern, the annular pattern provided for greater cell spreading thereby increasing the distance of the focal adhesions from the cell's center. The adhesion strength analysis was accomplished by utilizing hydrodynamic shear flow in a spinning disk device that was previously developed. The results indicate that for a constant total adhesive area, the annular patterns provide for greater adhesion strength by enhancing cell spreading area and providing for greater moment arm in resisting detachment due to shear. The next examination was the effect of the cell's internal force balance in stabilizing the cell adhesion. The working hypothesis was that microtubules provide the necessary forces to resist the tensile forces expressed by the cell contractile machinery, thereby stabilizing cell adhesion. Since microtubule disruption is known to enhance cell contractility, its effect on the cell adhesion strength was examined. Moreover, the force balance in cells was altered by engineering adhesive areas so that the cells were either spherical or completely spread and then disrupted microtubules to understand the significance of the force balance in modulating the cell adhesion strength. The results indicated that disruption of microtubules in cells on adhesive islands resulted in a 10 fold decrease in adhesion strength compared to untreated controls whereas no significant change was observed in completely spread cells between treated and untreated controls. This is in surprising contrast to the previous contractility inhibition studies which indicate a less pronounced regulation of adhesion strength for both micropatterned and spread cells. Taken together, these findings suggest that the internal force balance regulated by cell shape strongly modulates the adhesion strength though the microtubule network. In summary, this project elucidates the role of peripheral focal adhesions in regulating the cell adhesion strength. Furthermore, this study also establishes the importance of the internal force balance towards stabilizing the cell adhesion to the ECM through the microtubule network.
|
Page generated in 0.0565 seconds