Your search keyword '"Michiko Shimoda"' showing total 5 results

1. Interferon-signaling pathways are upregulated in people with HIV with abnormal pulmonary diffusing capacity (DLCO).

Author

Zhang, Michelle, Guorui Dai, Smith, Dana L., Zacco, Emanuela, Michiko Shimoda, Kumar, Nitasha, Girling, Valerie, Gardner, Kendall, Hunt, Peter W., Huang, Laurence, and Jue Lin

Published

2024

2. Metastasis of cholangiocarcinoma is promoted byextended high-mannose glycans.

Author

Park a, Diane Dayoung, b, Chatchai Phoomak, a, Gege Xu, Olney c, Laura P., Tran c, Khiem A., Park d, Simon S., Haigh c, Nathan E., c, Guillaume Luxardi, b, Worachart Lert-itthiporn, c, Michiko Shimoda, a, Qiongyu Li, e, Nobuyuki Matoba, f, Fernando Fierro, b, Sopit Wongkham, c, Emanual Maverakis, and Lebrilla a, Carlito B.

Subjects

MEMBRANE proteins, BILIARY tract cancer, GLYCANS, MEMBRANE glycoproteins, TRANSFERRIN receptors

Abstract

Membrane-bound oligosaccharides form the interfacial boundary between the cell and its environment, mediating processes such as adhesion and signaling. These structures can undergo dynamic changes in composition and expression based on cell type, external stimuli, and genetic factors. Glycosylation, therefore, is a promising target of therapeutic interventions for presently incurable forms of advanced cancer. Here, we show that cholangiocarcinoma metastasis is characterized by down-regulation of the Golgiα-mannosidase I coding gene MAN1A1, leading to elevation of extended high-mannose glycans with terminatingα-1,2-mannose residues. Subsequent reshaping of the gly come by in hibitingα-mannosidase Iresulted in significantly higher migratory and invasive capabilities while masking cell surface mannosylation suppressed metastasis-related pheno types. Exclusive elucidation of differentially expressed membrane glycoproteins and molecular modeling suggested that extended high-mannose glycosylation at the helical domain of transferrin receptor protein 1 promotes conformational changes that improve noncovalent interaction energies and lead to enhancement of cell migration in metastatic cholangiocarcinoma. The results provide support thatα-1,2-mannosylatedN-glycans present on cancer cell membrane proteins may serve as therapeutic targets for preventing metastasis. [ABSTRACT FROM AUTHOR]

Published

2020

3. Tunable hydrogels for mesenchymal stem cell delivery: Integrin-induced transcriptome alterations and hydrogel optimization for human wound healing.

Author

Marusina, Alina I., Merleev, Alexander A., Luna, Jesus I., Olney, Laura, Haigh, Nathan E., Yoon, Daniel, Chen Guo, Ovadia, Elisa M., Michiko Shimoda, Luxardi, Guillaume, Boddu, Sucharita, Lal, Nelvish N., Yoshikazu Takada, Lam, Kit S., Ruiwu Liu, Isseroff, R. Rivkah, Le, Stephanie, Nolta, Jan A., Kloxin, April M., and Maverakis, Emanual

Subjects

HYDROGELS, MESENCHYMAL stem cells, INTEGRINS, TRANSCRIPTOMES, WOUND healing

Abstract

Therapeutic applications for mesenchymal stem/stromal cells (MSCs) are growing; however, the successful implementation of these therapies requires the development of appropriate MSC delivery systems. Hydrogels are ideally suited to cultivate MSCs but tuning hydrogel properties to match their specific in vivo applications remains a challenge. Thus, further characterization of how hydrogel-based delivery vehicles broadly influence MSC function and fate will help lead to the next generation of more intelligently designed delivery vehicles. To date, few attempts have been made to comprehensively characterize hydrogel impact on the MSC transcriptome. Herein, we have synthesized cell-degradable hydrogels based on bio-inert poly(ethylene glycol) tethered with specific integrin-binding small molecules and have characterized their resulting effect on the MSC transcriptome when compared with 2D cultured and untethered 3D hydrogel cultured MSCs. The 3D culture systems resulted in alterations in the MSC transcriptome, as is evident by the differential expression of genes related to extracellular matrix production, glycosylation, metabolism, signal transduction, gene epigenetic regulation, and development. For example, genes important for osteogenic differentiation were upregulated in 3D hydrogel cultures, and the expression of these genes could be partially suppressed by tethering an integrin-binding RGD peptide within the hydrogel. Highlighting the utility of tunable hydrogels, when applied to ex vivo human wounds the RGD-tethered hydrogel was able to support wound re-epithelialization, possibly due to its ability to increase PDGF expression and decrease IL-6 expression. These results will aid in future hydrogel design for a broad range of applications. [ABSTRACT FROM AUTHOR]

Published

2020

4. CD4 memory T cells develop and acquire functional competence by sequential cognate interactions and stepwise gene regulation.

Author

Tomohiro Kaji, Atsushi Hijikata, Akiko Ishige, Toshimori Kitami, Takashi Watanabe, Osamu Ohara, Noriyuki Yanaka, Mariko Okada, Michiko Shimoda, Masaru Taniguchi, and Toshitada Takemori

Subjects

CD4 antigen, T cell differentiation, GENETIC regulation, HUMORAL immunity, HOMEOSTASIS, GENETIC markers

Abstract

Memory CD4+ T cells promote protective humoral immunity; however, how memory T cells acquire this activity remains unclear. This study demonstrates that CD4+ T cells develop into antigen-specific memory T cells that can promote the terminal differentiation of memory B cells far more effectively than their naive T-cell counterparts. Memory T cell development requires the transcription factor B-cell lymphoma 6 (Bcl6), which is known to direct T-follicular helper (Tfh) cell differentiation. However, unlike Tfh cells, memory T cell development did not require germinal center B cells. Curiously, memory T cells that develop in the absence of cognate B cells cannot promote memory B-cell recall responses and this defect was accompanied by down-regulation of genes associated with homeostasis and activation and up-regulation of genes inhibitory for T-cell responses. Although memory T cells display phenotypic and genetic signatures distinct from Tfh cells, both had in common the expression of a group of genes associated with metabolic pathways. This gene expression profile was not shared to any great extent with naive T cells and was not influenced by the absence of cognate B cells during memory T cell development. These results suggest that memory T cell development is programmed by stepwise expression of gatekeeper genes through serial interactions with different types of antigen-presenting cells, first licensing the memory lineage pathway and subsequently facilitating the functional development of memory T cells. Finally, we identified Gdpd3 as a candidate genetic marker for memory T cells. [ABSTRACT FROM AUTHOR]

Published

2016

5. Persistence of Autoreactive IgA-Secreting B Cells Despite Multiple Immunosuppressive Medications Including Rituximab.

Author

Yong He, Michiko Shimoda, Yoko Ono, Villalobos, Itzel Bustos, Mitra, Anupam, Konia, Thomas, Grando, Sergei A., Zone, John J., and Maverakis, Emanual

Published

2015