458 First phase 2 results of autologous tumor-infiltrating lymphocyte (TIL; LN-145) monotherapy in patients with advanced, immune checkpoint inhibitor-treated, non-small cell lung cancer (NSCLC)

Schoenfeld, Adam J.; Lee, Sylvia; Paz‐Ares, Luis; Doger, Bernard; Gettinger, Scott; Haefliger, Simon; Orcurto, Angela; Sukari, Ammar; Papa, Sophie; Moreno, Juan Francisco Rodriguez; Finckenstein, Friedrich Graf; Jagasia, Madan; Fiaz, Rana; Sulur, Giri; Chen, Guang; Gontcharova, Viktoria; He, Kai

doi:10.1136/jitc-2021-sitc2021.458

Cited by 20 publications

(26 citation statements)

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“… 6 Recently, in a multicenter phase II study of patients with advanced NSCLC, more than 50% of lesions resected were from the lung, and patients could be administered therapeutic TIL doses with minimal morbidity. 16 The feasibility of TIL production from NSCLC tumors was also demonstrated in a phase I study, in which adequate tumor tissue was collected from excisional biopsy of metastases in pleural nodules or supraclavicular lymph nodes, with most patients discharged within a day following the biopsy procedure. 15 …”

Section: Tumor/surgical Site Selection and Considerationsmentioning

confidence: 99%

“…Further, the in vivo fate of individual TIL clones is not dependent on their frequency in the infusion product, as minor clones within the infusion product can expand preferentially after infusion, hypothetically reflecting antigen-driven clonal proliferation 51 . The TCR repertoire of TILs (LN-145) generated from NSCLC tumors of patients with advanced NSCLC demonstrated a highly polyclonal product with unique TCR clones, as indicated by the Shannon Entropy Index and Simpson Clonality Index 16 . The number of unique TCR clones obtained from NSCLC tumors, as well as measures of diversity and clonality, was similar to those previously published for lifileucel for melanoma 51 and LN-145 for cervical cancer 52 .…”

Section: Tumor Resection Site Does Not Influence Tcr Repertoirementioning

confidence: 99%

“…As TIL cell therapy approaches commercialization, standardized protocols are required. Recent multicenter studies in advanced melanoma, HNSCC, cervical cancer, and NSCLC represent a major advance in this respect 6,12,16 . These studies benefit from a centralized Good Manufacturing Practice process, which allows for timely delivery of therapy and facilitates the production of reproducible high-quality TIL cell therapy products for broader patient accessibility.…”

Section: Advances In Til Manufacturing Processmentioning

confidence: 99%

“… 45 , 46 The operating surgeon is best qualified to prosect and select the most viable tumor tissue for optimal TIL production. Although no formal minimal size criteria have been established for resection of viable solid tumor tissue, some studies and trials in progress recommend a postprosection aggregate tumor tissue diameter of 1 cm or greater 47 or 1.5 cm or greater but less than 4 cm, 6 , 16 , 48 whereas others recommend a metastatic tumor tissue of 1 cm 3 or greater (>2 cm 3 for lymph nodes). 7 If the volume of tissue from 1 lesion is not adequate, an additional lesion can be resected to make up the size specifications, with 1.5 cm or greater in aggregate diameter after trimming to meet the minimum TIL manufacturing requirements.…”

Section: Additional Tumor Tissue Considerationsmentioning

confidence: 99%

“…Adoptive cell therapy using investigational TIL cell therapy has demonstrated encouraging efficacy and safety in clinical trials for several patient populations with high unmet medical need, including advanced melanoma, 6 , 8 – 13 non–small cell lung cancer (NSCLC), 14 – 16 cervical cancer, 12 , 17 and head and neck squamous cell carcinoma (HNSCC). 12 , 18 Most of these studies included heavily pretreated patients who had failed all prior therapies and had limited treatment options.…”

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confidence: 99%

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Surgical Considerations for Tumor Tissue Procurement to Obtain Tumor-Infiltrating Lymphocytes for Adoptive Cell Therapy

et al. 2022

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Adoptive cell therapy with tumor-infiltrating lymphocytes (TILs), an investigational cellular therapy, has demonstrated antitumor efficacy in patients with advanced solid tumors, including melanoma. Tumor-infiltrating lymphocyte cell therapy involves surgical resection of a patient's tumor, ex vivo TIL expansion under conditions that overcome immunosuppressive responses elicited by the tumor and the tumor microenvironment, administration of a lymphodepleting regimen, and infusion of the final TIL cell therapy product back into the patient followed by interleukin 2 administration to support T-cell activity. The surgeon plays a central role in patient identification and tumor selection—steps that are critical for successful outcomes of TIL cell therapy. Commercialization of TIL cell therapy and its broader access to patients will require education and collaboration among surgeons, oncologists, and cellular therapists. This review highlights the unique role that surgeons will play in the implementation of TIL cell therapy and serves as a contemporary report of best practices for patient selection and tumor resection methods.

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Section: Tumor/surgical Site Selection and Considerationsmentioning

confidence: 99%

Section: Tumor Resection Site Does Not Influence Tcr Repertoirementioning

confidence: 99%

Section: Advances In Til Manufacturing Processmentioning

confidence: 99%

Section: Additional Tumor Tissue Considerationsmentioning

confidence: 99%

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confidence: 99%

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Surgical Considerations for Tumor Tissue Procurement to Obtain Tumor-Infiltrating Lymphocytes for Adoptive Cell Therapy

et al. 2022

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Tumor‐infiltrating lymphocyte therapy: Clinical aspects and future developments in this breakthrough cancer treatment

Lee

Kim²,

Chung³

et al. 2023

BioEssays

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Tumor‐infiltrating lymphocyte (TIL) therapy is a promising approach for treating refractory or advanced solid cancers by using autologous TILs harvested from cancer tissues. Despite the heterogeneity of cancer, TIL therapy can potentially produce a positive therapeutic response, including complete remission. After decades of research on lymphocyte functions, culture/expansion methods, therapeutic protocols, and multiple clinical trials, TIL therapy has finally reached a stage where it can be formally approved for clinical use. TIL therapy is expected to hold a unique position among anti‐cancer therapeutic options as a standard intervention. To successfully introduce TIL therapy into clinical settings, there is a need to expand therapeutic indications and set up the best protocols for cancer tissue sampling and manufacturing, and related clinical trials. Moreover, studies on next‐generation TIL therapy have already begun, and post‐approval real‐world data will promote and support further research.

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Modulation of intracellular kinase signaling to improve TIL stemness and function for adoptive cell therapy

Feng

Qiu

Shi³

et al. 2022

Cancer Medicine

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Introduction Adoptive cellular therapy with tumor‐infiltrating lymphocytes (TIL) has demonstrated promising clinical benefits in several solid tumors, but the efficacy of this therapy might be compromised by the “prone‐to‐exhaustion” phenotype of TIL and poor persistence in vivo. This calls for a robust expansion process to produce a large number of cells for clinical usage while at the same time maintaining favorable anti‐tumor function and memory phenotype. Previous studies showed that the PI3K‐AKT signaling pathway plays a key role in the regulation of T cell activation, differentiation and memory formation. Method We modulated the PI3K‐AKT pathway in TIL isolated from cervical and ovarian cancer by application of AKT or PI3K inhibitors or CRISPR knockout of AKT1 and/or AKT2, and characterized their effects on TIL phenotype and effector function. Mechanistic study was further performed with RNA‐seq analysis of AKT1/2 KO TIL in comparison to control TIL. Result The inhibition of either PI3K or AKT led to an increase in the population of effector CD8 + T cells with upregulation of activation markers, elevated CD39 − CD69 − memory T cells, and significantly enhanced cytotoxicity when cocultured with tumor cell lines and patient‐derived tumor samples. Moreover, dual knockout of AKT1 and AKT2 largely phenocopies the functional impact of AKT or PI3K inhibition on TIL. This result was further validated by RNA‐seq analysis indicating that AKT1/2 ablation primarily regulates T cell differentiation and function‐related programs. Conclusion Modulation of PI3K‐AKT signaling represents a promising strategy to enhance TIL stemness and cytotoxicity and improve the clinical outcome of current TIL‐based therapy to treat solid tumors.

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458 First phase 2 results of autologous tumor-infiltrating lymphocyte (TIL; LN-145) monotherapy in patients with advanced, immune checkpoint inhibitor-treated, non-small cell lung cancer (NSCLC)

Cited by 20 publications

References 1 publication

Surgical Considerations for Tumor Tissue Procurement to Obtain Tumor-Infiltrating Lymphocytes for Adoptive Cell Therapy

Surgical Considerations for Tumor Tissue Procurement to Obtain Tumor-Infiltrating Lymphocytes for Adoptive Cell Therapy

Tumor‐infiltrating lymphocyte therapy: Clinical aspects and future developments in this breakthrough cancer treatment

Modulation of intracellular kinase signaling to improve TIL stemness and function for adoptive cell therapy

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