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Featured researches published by Wajeeh Saadi.


Annals of Biomedical Engineering | 2005

Neutrophil migration in opposing chemoattractant gradients using microfluidic chemotaxis devices.

Francis Lin; Connie Minh-Canh Nguyen; Shur-Jen Wang; Wajeeh Saadi; Steven P. Gross; Noo Li Jeon

Neutrophils migrating in tissue respond to complex overlapping signals generated by a variety of chemotactic factors (CFs). Previous studies suggested a hierarchy between bacteria-derived CFs and host-derived CFs but could not differentiate neutrophil response to potentially equal host-derived CFs (IL-8 and LTB4). This paper reports neutrophil migration in conflicting gradients of IL-8 and LTB4 using a microfluidic chemotaxis device that can generate stable and well-defined gradients. We quantitatively characterized the movement of cells from time-lapse images. Neutrophils migrate more efficiently toward single IL-8 gradients than single LTB4 gradients as measured by the effective chemotactic index (ECI). In opposing gradients of IL-8 and LTB4, neutrophils show obvious chemotaxis toward a distant gradient, consistent with previous reports. When an opposing gradient of LTB4 is present, neutrophils show less effective chemotaxis toward IL-8 than when they are in a gradient of IL-8 alone. In contrast, the chemotactic response of neutrophils to LTB4 is not reduced in opposing gradients as compared to that in a single LTB4 gradient. These results indicate that the presence of one host-derived CF modifies the response of neutrophils to a second CF suggesting a subtle hierarchy between them.


Biotechnology and Bioengineering | 2008

Epidermal growth factor promotes breast cancer cell chemotaxis in CXCL12 gradients.

Bobak Mosadegh; Wajeeh Saadi; Shur-Jen Wang; Noo Li Jeon

The chemokine receptor CXCR4 and its ligand CXCL12 play an important role in breast cancer invasion and metastasis, and induce the chemotaxis of various types of cancer cells. Previous studies of CXCL12‐induced chemotaxis have, for the most part, relied on endpoint assays (e.g., transwell assays) that provide poor control over the cell microenvironment. Specifically, these assays lacked the ability to dissect the role that autocrine and paracrine growth factors play in chemokine‐induced cancer cell chemotaxis. Here, we employ a microfluidic chemotaxis chamber that allows the effects of specific exogenous factors on cell migration to be directly characterized, without the interference of autocrine/paracrine signaling. Using this approach, we investigated the migration of MDA‐MB‐231 breast cancer cells in well‐defined CXCL12 gradients. We found that CXCL12 alone failed to stimulate chemotaxis of these cells; however, when the CXCL12 gradient was supplemented with a uniform stimulus of either EGF or conditioned media, a directional response was induced. This dependence on growth factor signaling points to the importance of autocrine and paracrine factors in determining the migratory response of the cells, and may play an important role in cancer metastasis. Biotechnol. Bioeng. 2008;100: 1205–1213.


Journal of Visualized Experiments | 2007

A Gradient-generating Microfluidic Device for Cell Biology

Bong Geun Chung; Amir Manbachi; Wajeeh Saadi; Francis Lin; Noo Li Jeon; Ali Khademhosseini

The fabrication and operation of a gradient-generating microfluidic device for studying cellular behavior is described. A microfluidic platform is an enabling experimental tool, because it can precisely manipulate fluid flows, enable high-throughput experiments, and generate stable soluble concentration gradients. Compared to conventional gradient generators, poly(dimethylsiloxane) (PDMS)-based microfluidic devices can generate stable concentration gradients of growth factors with well-defined profiles. Here, we developed simple gradient-generating microfluidic devices with three separate inlets. Three microchannels combined into one microchannel to generate concentration gradients. The stability and shape of growth factor gradients were confirmed by fluorescein isothyiocyanate (FITC)-dextran with a molecular weight similar to epidermal growth factor (EGF). Using this microfluidic device, we demonstrated that fibroblasts exposed to concentration gradients of EGF migrated toward higher concentrations. The directional orientation of cell migration and motility of migrating cells were quantitatively assessed by cell tracking analysis. Thus, this gradient-generating microfluidic device might be useful for studying and analyzing the behavior of migrating cells.


Experimental Cell Research | 2004

Differential effects of EGF gradient profiles on MDA-MB-231 breast cancer cell chemotaxis

Shur-Jen Wang; Wajeeh Saadi; Francis Lin; Connie Minh-Canh Nguyen; Noo Li Jeon


Biomedical Microdevices | 2007

Generation of stable concentration gradients in 2D and 3D environments using a microfluidic ladder chamber

Wajeeh Saadi; Seog Woo Rhee; Francis Lin; Behrad Vahidi; Bong Geun Chung; Noo Li Jeon


Lab on a Chip | 2004

Generation of dynamic temporal and spatial concentration gradients using microfluidic devices

Francis Lin; Wajeeh Saadi; Seog Woo Rhee; Shur-Jen Wang; Sukant Mittal; Noo Li Jeon


Biomedical Microdevices | 2006

A parallel-gradient microfluidic chamber for quantitative analysis of breast cancer cell chemotaxis

Wajeeh Saadi; Shur-Jen Wang; Francis Lin; Noo Li Jeon


Biochemical and Biophysical Research Communications | 2004

Effective neutrophil chemotaxis is strongly influenced by mean IL-8 concentration

Francis Lin; Connie Minh-Canh Nguyen; Shur-Jen Wang; Wajeeh Saadi; Steven P. Gross; Noo Li Jeon


Archive | 2007

Microfluidic gradient devices

Noo Li Jeon; Wajeeh Saadi; Seog Woo Rhee; Bobak Mosadegh; Carlos P. Huang


IEEE Transactions on Biomedical Engineering | 2005

Neutrophil Migration in Opposing Chemoattractant Gradients Using Microfluidic Chemotaxis Devices

Frank Yeong-sung Lin; Connie Minh-Canh Nguyen; Shur-Jen Wang; Wajeeh Saadi; Steven G. Ross; Noo Li Jeon

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Noo Li Jeon

Seoul National University

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Shur-Jen Wang

University of California

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Francis Lin

University of Manitoba

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Seog Woo Rhee

Kongju National University

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Behrad Vahidi

University of California

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