New cytometry tools for immune monitoring during cancer immunotherapy

Sanjabi, Shomyseh; Lear, Sean

doi:10.1002/cyto.b.21984

Cited by 11 publications

(7 citation statements)

References 67 publications

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“…Numerous studies have demonstrated that an elevated frequency of CD4+CD25+FoxP3+ T (Treg) cells play the role of negative immune regulation in solid tumors and hematological malignancies (Dehghani et al, 2021; Saleh & Elkord, 2020; Zheng et al, 2011). It is showed that the PD‐1/PD‐L1 axis functions as an immune checkpoint against unrestrained cytotoxic T effector cell activity‐it promotes peripheral T effector cell exhaustion and conversion of T effector cells to immunosuppressive Tregs (Park et al, 2020; Sanjabi & Lear, 2021). Increasing numbers of Tregs may accelerate T cell senescence and exhaustion and associated with high mortality and reduced survival time (Fu et al, 2007; Tang et al, 2020).…”

Section: Discussionmentioning

confidence: 99%

Increased TOX expression concurrent with PD‐1, Tim‐3, and CD244 expression in T cells from patients with acute myeloid leukemia

Huang

Liang

Zhao

et al. 2021

Cytometry Part B Clinical

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Background T cell dysregulation is a common event in leukemia. Recent findings have indicated that aberrant expression of immune checkpoint proteins may be associated with disease relapse and progression in acute myeloid leukemia (AML). TOX, a transcription factor in the HMG‐box protein superfamily, was found to be a potential target for immunotherapy not only in solid tumors but also in hematological malignancies. However, little is known about TOX expression and co‐expression with immune checkpoint proteins or the exhausted phenotype in the T cell subsets in AML. Thus, in this study, we analyzed TOX expression and co‐expression with PD‐1, Tim‐3, and CD244 in T cells. Methods TOX expression and co‐expression with PD‐1, Tim‐3, and CD244 in CD3+, CD4+, regulatory T (Treg), and CD8+ T cells were analyzed by multi‐color fluorescent flow cytometry in peripheral blood (PB) and bone marrow (BM) samples from patients with de novo AML and AML in complete remission (CR) and healthy individuals (HIs). Results A significantly increased percentage of TOX+CD3+, CD4+, and CD8+ T cells was found in PB from patients with de novo AML in comparison with HIs. Double‐positive TOX+CD244+, TOX+PD‐1+, and TOX+Tim‐3+ T cells markedly increased in the CD3+, CD4+, and CD8+ T cell populations in de novo AML patients compared with HIs, and similar trends were demonstrated for TOX+Tim‐3+CD3+/CD4+/CD8+ T cells in de novo AML compared with AML‐CR patients. In addition, the number of TOX+, TOX+PD‐1+, and TOX+Tim‐3+Treg cells significantly increased in de novo AML patients compared with HIs, and TOX+PD‐1+Treg cells were higher in de novo AML compared with AML‐CR patients. Moreover, TOX positively correlated with Tim‐3 expression in CD8+ and Treg cells, and a positive correlation between the expression of TOX+ CD4+ and CD244+CD4+ T cells was found. Furthermore, an increased percentage of TOX+Tim‐3+ T cells in BM was also found in de novo AML patients compared with HIs. Conclusions Increased TOX concurrent with PD‐1, Tim‐3, and CD244 in T cells may contribute to T cell exhaustion and impair their function in AML. Such exhausted T cells may be partially revised when AML patients achieve CR after chemotherapy. TOX may be considered a potential target for reversing T cell exhaustion and improving T cell function in AML.

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Section: Discussionmentioning

confidence: 99%

Increased TOX expression concurrent with PD‐1, Tim‐3, and CD244 expression in T cells from patients with acute myeloid leukemia

Huang

Liang

Zhao

et al. 2021

Cytometry Part B Clinical

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“…We enrolled aHCC patients who were also subjects of the Checkmate-040 trial from National Taiwan University Hospital (Taipei, Taiwan) and Taipei Veteran General Hospital (Taipei, Taiwan). Eligible criteria included: (1) older than 20 years old, (2) histological confirmed aHCC based on the practical guideline, (3) Child-Pugh class A, (4) Eastern Cooperative Oncology Group (ECOG) performance status 0 or 1, (5) adequate organ function for Checkmate-040 trial, (6) plan to receive nivolumab treatment, (7) no therapeutic modalities within four weeks prior to initial dose of nivolumab, and (8) did not receive any immuno-modulating medications. Patients who did not sign the informed consent form were ineligible.…”

Section: Methodsmentioning

confidence: 99%

“…Flow cytometry allows a detailed single-cell characterization of adaptive and innate immune landscapes, thereby providing a unique platform to discriminate immune cell subsets that can be exploited in an immunotherapeutic setting ( 7 ). Previously, we conducted an observational study to screen the immune cell subsets of aHCC patients and identified a significantly lower percentage of PD-1 + B cells in peripheral blood mononuclear cells (PBMCs) from aHCC patients with disease progression responses than those with disease control response after nivolumab treatment ( 8 , 9 ).…”

Section: Introductionmentioning

confidence: 99%

Artificial intelligence-based immunoprofiling serves as a potentially predictive biomarker of nivolumab treatment for advanced hepatocellular carcinoma

Lee¹,

Hung²,

Chou³

et al. 2022

Front. Med.

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Immune checkpoint inhibitors (ICI) have been applied in treating advanced hepatocellular carcinoma (aHCC) patients, but few patients exhibit stable and lasting responses. Moreover, identifying aHCC patients suitable for ICI treatment is still challenged. This study aimed to evaluate whether dissecting peripheral immune cell subsets by Mann-Whitney U test and artificial intelligence (AI) algorithms could serve as predictive biomarkers of nivolumab treatment for aHCC. Disease control group carried significantly increased percentages of PD-L1+ monocytes, PD-L1+ CD8 T cells, PD-L1+ CD8 NKT cells, and decreased percentages of PD-L1+ CD8 NKT cells via Mann-Whitney U test. By recursive feature elimination method, five featured subsets (CD4 NKTreg, PD-1+ CD8 T cells, PD-1+ CD8 NKT cells, PD-L1+ CD8 T cells and PD-L1+ monocytes) were selected for AI training. The featured subsets were highly overlapping with ones identified via Mann-Whitney U test. Trained AI algorithms committed valuable AUC from 0.8417 to 0.875 to significantly separate disease control group from disease progression group, and SHAP value ranking also revealed PD-L1+ monocytes and PD-L1+ CD8 T cells exclusively and significantly contributed to this discrimination. In summary, the current study demonstrated that integrally analyzing immune cell profiling with AI algorithms could serve as predictive biomarkers of ICI treatment.

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“…There is an increasing interest in profiling immune cell populations in tumor sites and peripheral blood and correlating this with therapy response and/or toxicities (Greenplate et al, 2016). As flow cytometry is expanding its multicolour capabilities, new studies aiming at an in-depth in site immune evaluation are needed (Sanjabi & Lear, 2021).…”

Section: Evaluation Of Immune Cell Populations In Infiltrated Versus ...mentioning

confidence: 99%

Routine flow cytometry approach for the evaluation of solid tumor neoplasms and immune cells in minimally invasive samples

Quirós

Fernández

Fonseca-Mourelle

et al. 2022

Cytometry Part B Clinical

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Background: Multidimensional flow cytometry (MFC) is routinely used for the diagnosis and follow-up of hematolymphoid neoplasms but its contribution to the identification of non-hematolymphoid malignant tumors is limited. Methods:The presence of non-hematolymphoid cells in clinical samples obtained via minimally invasive methods was ascertained by using a panel of monoclonal antibodies previously developed in our laboratory comprising a mixture of antibodies: CD9-PacB/CD45-OC515/CD57-FITC/CD56-PE/CD3-PerCP-Cy5.5/CD117-PE-Cy7/CD326-APC/CD81-APC-C750. Histopathological studies were performed using standard techniques.Results: 164 specimens of different origins were included. Malignancy was finally confirmed in 142 (86.5%), while 22 non neoplastic samples were identified. The most frequent diagnosis was small cell lung carcinoma (SCLC) (50%). High sensitivity (S = 98.6%) was reached combining MFC and conventional pathology. Individual markers differed according to the cellular origin of the neoplasm, with neuroendocrine tumors showing a unique immunophenotypic profile (CD56+ CD326+ CD117À/+ and variable tetraspanins expression). Principal component analysis efficiently distinguished SCLC from other tumor samples. In immune cell populations, differences between reactive and malignant biopsies were found in different cell compartments, especially in B cells and Plasma cells. Differences also emerged in the percentage of CD4+ CD8À T cells, CD4-CD8+ T cells and NK cells and these were dependent on the origin of the tumor cells.Conclusions: These results support the use of MFC as a rapid and valuable technique to detect non-hematolymphoid tumoral cells in clinical specimens, providing an initial orientation to complement hystopathological studies and allow a more precise diagnosis, especially in neuroendocrine neoplasms. The impact of different immune cell patterns warrants further research.

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New cytometry tools for immune monitoring during cancer immunotherapy

Cited by 11 publications

References 67 publications

Increased TOX expression concurrent with PD‐1, Tim‐3, and CD244 expression in T cells from patients with acute myeloid leukemia

Increased TOX expression concurrent with PD‐1, Tim‐3, and CD244 expression in T cells from patients with acute myeloid leukemia

Artificial intelligence-based immunoprofiling serves as a potentially predictive biomarker of nivolumab treatment for advanced hepatocellular carcinoma

Routine flow cytometry approach for the evaluation of solid tumor neoplasms and immune cells in minimally invasive samples

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