自引率: 5.5%
被引量: 6557
通过率: 暂无数据
审稿周期: 2.67
版面费用: 暂无数据
国人发稿量: 42
投稿须知/期刊简介:
Published by Taylor and Francis Group. ISSN: 1465-3249.<br /><br />Cytotherapy aims to bring readers the very latest developments in the fast-moving field of cellular therapies, and to educate readers in their medical application. Areas covered include cytotherapy, biology of transplantation, stem cell studies, immunotherapy, gene therapy and clinical transplantation, as well as the science, management and operation of the laboratory. The journal reflects the diverse sciences within the field, and with full-colour illustrations, figures, flow charts and photographs, it is an excellent tool for the dissemination of the most recent developments across the area.
期刊描述简介:
Published by Taylor and Francis Group. ISSN: 1465-3249. Cytotherapy aims to bring readers the very latest developments in the fast-moving field of cellular therapies, and to educate readers in their medical application. Areas covered include cytotherapy, biology of transplantation, stem cell studies, immunotherapy, gene therapy and clinical transplantation, as well as the science, management and operation of the laboratory. The journal reflects the diverse sciences within the field, and with full-colour illustrations, figures, flow charts and photographs, it is an excellent tool for the dissemination of the most recent developments across the area.
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The role of the conditioning regimen for autologous and ex vivo genetically modified hematopoietic stem cell-based therapies: recommendations from the ISCT stem cell engineering committee.
被引量:- 发表:1970
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Comprehensive analysis of secretome and transcriptome stability of Wharton jelly mesenchymal stromal cells during good manufacturing practice-compliant production.
被引量:- 发表:1970
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Comprehensive characterization of cytopenia after chimeric antigen receptor-T cell infusion in patients with relapsed or refractory multiple myeloma.
被引量:- 发表:1970
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Expansion of tumor-infiltrating and marrow-infiltrating lymphocytes from pediatric malignant solid tumors.
The expansion of tumor-infiltrating lymphocytes (TIL) for adoptive cellular therapy is under investigation in many solid tumors of adulthood. Marrow-infiltrating lymphocytes (MIL) have demonstrated antitumor reactivity preclinically. Successful expansion of TIL/MIL has not been reported across pediatric solid tumor histologies. The objective of this study was to demonstrate successful expansion of TIL from pediatric solid tumors for translation in an adoptive cell therapy (ACT) treatment strategy. A prospective study of TIL/MIL expansion was performed on solid tumors of pediatric patients undergoing standard-of-care procedures. TIL/MIL expansions were performed in the presence of high-dose interleukin 2. To demonstrate a full-scale expansion to clinically-relevant cell doses for TIL therapy, initial TIL culture was followed by a rapid expansion protocol for select patients. Expanded specimens were analyzed for phenotype by flow cytometry and for anti-tumor reactivity by the interferon-gamma release assay. Eighteen tumor samples were obtained. Initial TIL cultures were successfully generated from 14/18 samples (77.7%). A median of 5.52 × 107 (range: 2.5 × 106-3.23 × 108) cells were produced from initial cultures, with 46.9% expressing a CD3 phenotype (46.9%). Eight samples underwent rapid expansion, demonstrating a median 458-fold expansion and a CD3 phenotype of 98%. Initial MIL cultures were successfully generated from five samples, with a predominantly CD3 phenotype (45.2%). Sufficient tumor tissue was only available for seven TIL samples to be tested for reactivity; none demonstrated responsiveness to autologous tumor. TIL and MIL expansion from pediatric solid tumors was successful, including the full-scale expansion process. This data supports translation to an ACT-TIL treatment strategy in the pediatric population and thus a Phase I trial of ACT-TIL in pediatric high-risk solid tumors is planned.
被引量:1 发表:1970
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CD19 CAR-T treatment shows limited efficacy in r/r DLBCL with double expression and TP53 alterations.
Autologous CD19 chimeric antigen receptor T-cell therapy (CAR-T) significantly modifies the natural course of chemorefractory diffuse large B-cell lymphoma (DLBCL). However, 25% to 50% of patients with relapsed/refractory DLBCL still do not achieve remission. Therefore, investigating new molecular prognostic indicators that affect the effectiveness of CAR-T for DLBCL and developing novel combination therapies are crucial. Data from 73 DLBCL patients who received CD19 CAR-T (Axi-cel or Relma-cel) were retrospectively collected from Shanghai Tongji Hospital of Tongji University, The Second Affiliated Hospital Zhejiang University School of Medicine, and The Affiliated People's Hospital of Ningbo University. Prior to CD19 CAR-T-cell transfusions, the patients received fludarabine and cyclophosphamide chemotherapy regimen. Our study revealed that relapsed/refractory diffuse large B-cell lymphoma (r/r DLBCL) patients with both Double-expression (MYC > 40% and BCL2 > 50%) and TP53 alterations tend to have a poorer clinical prognosis after CAR-T therapy, even when CAR-T therapy is used in combination with other therapies. However, CAR-T therapy was found to be effective in patients with only TP53 alterations or DE status, suggesting that their prognosis is in line with that of patients without TP53 alterations or DE status. Our study suggests that r/r DLBCL patients with both DE status and TP53 alterations treated with CAR-T therapy are more likely to have a poorer clinical prognosis. However, CAR-T therapy has the potential to improve the prognosis of patients with only TP53 alterations or DE status to be similar to that of patients without these abnormalities.
被引量:- 发表:1970
