Publications by authors named "Toyoshi Matsutake"

Lung spindle cell carcinoma is an aggressive subtype of pleomorphic lung cancer resistant to cytotoxic chemotherapy. Programmed cell death-1 (PD-1) inhibitors have been reported to have clinical effects in patients with spindle cell carcinoma; however, the resistance mechanism to PD-1 inhibitors is yet to be fully elucidated. Herein, we report the case of an 88-year-old man with G-CSF-producing spindle cell carcinoma who acquired resistance to PD-1/PD-ligand 1 (L1) inhibitor in an early setting after a remarkable response.

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Article Synopsis
  • * A thoracoscopy revealed an unexpected pleural mass on the parietal pleura, which was completely removed.
  • * The mass was diagnosed as pleural capillary hemangioma, and after its removal, the effusion did not return, highlighting hemangioma as a key diagnosis for persistent pleural effusions.
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In this study, we used "RAPIRUN(®)Streptococcus pneumoniae HS (otitis media/sinusitis) (RAPIRUN-HS)," a rapid S. pneumoniae antigen detection kit, to investigate methods for detecting S. pneumoniae antigens in blood of 32 bacterial pneumonia patients.

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A 66-year-old man was transferred to our hospital on November 2010 owing to a diagnosis of miliary tuberculosis. Treatment was initially started with INH, RFP, PZA, and EB. However, PZA and EB were discontinued because of their adverse effects.

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Exogenous antigens enter antigen-presenting cells through non-specific mechanisms and are presented by the MHC II molecules. We show here that antigens chaperoned by the heat shock protein gp96 enter dendritic cells and B cells through a specific, CD91- and LOX-1-mediated mechanism, and are presented by MHC II molecules, in addition to MHC I molecules as previously demonstrated. Receptor utilization results in high efficiency uptake such that antigen concentrations as low as 10(-9) M, if chaperoned by gp96, lead to productive antigen presentation.

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The heat shock protein-antigen presenting cell interaction lies at the center of the unique properties of heat shock proteins as immunogens. This interaction is a key event in adaptive immune response elicited by heat shock protein-chaperoned peptides, naturally derived or artificially reconstituted. The heat shock protein-antigen presenting cell interaction results in a primitive and fundamental chain of events, i.

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