Publications by authors named "J Mineno"

Article Synopsis
  • Adeno-associated virus (AAV) vectors are important for gene therapy but are produced with various impurities, making purification essential.
  • The study highlights the use of equilibrium density gradient analytical ultracentrifugation (DGE-AUC) to accurately quantify full and empty AAV particles, and to identify other components.
  • While DGE-AUC is effective for assessing particle density and purity, it has limitations in detecting minor components with low absorption or similar densities to major AAV components, thus complementing other methods like sedimentation velocity AUC (SV-AUC) and band sedimentation AUC (BS-AUC).
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Article Synopsis
  • - CAR-T therapy shows great promise for treating blood cancers but struggles with solid tumors due to unique challenges related to tumor microenvironments.
  • - This study utilized a mouse model of pancreatic ductal adenocarcinoma (PDAC) to investigate how CAR-T cells behave in solid tumors, revealing that these cells can actually persist and accumulate in PDAC tissues.
  • - Despite their presence, CAR-T cells exhibited a gradual loss of effectiveness against the tumor over time, linked to changes in specific proteins associated with cell metabolism and function.
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Adoptive immunotherapy using genetically engineered patient-derived lymphocytes to express tumor-reactive receptors is a promising treatment for malignancy. However, utilization of autologous T cells in this therapy limits the quality of gene-engineered T cells, thereby inhibiting the timely infusion of the cells into patients. In this study, we evaluated the anti-tumor efficacy and the potential to induce graft-versus-host disease (GVHD) in T cell receptor (TCR) gene-engineered allogeneic T cells that downregulate the endogenous TCR and HLA class I molecules with the aim of developing an "off-the-shelf" cell product with expanded application of genetically engineered T cells.

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Emerging SARS-CoV-2 Omicron variants are highly contagious with enhanced immune escape mechanisms against the initially approved COVID-19 vaccines. Therefore, we require stable alternative-platform vaccines that confer protection against newer variants of SARS-CoV-2. We designed an Omicron B.

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The benefits of CAR-T therapy could be expanded to the treatment of solid tumors through the use of derived autologous αβ T cell, but clinical trials of CAR-T therapy for patients with solid tumors have so far been disappointing. CAR-T therapy also faces hurdles due to the time and cost intensive preparation of CAR-T cell products derived from patients as such CAR-T cells are often poor in quality and low in quantity. These inadequacies may be mitigated through the use of third-party donor derived CAR-T cell products which have a potent anti-tumor function but a constrained GVHD property.

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