CD24 Is a Potential Immunotherapeutic Target for Mantle Cell Lymphoma

Freile, Jimena Álvarez; Avtenyuk, Natasha Ustyanovska; Corrales, Macarena González; Lourens, Harm Jan; Huls, Gerwin; Meerten, Tom van; Cendrowicz, Ewa; Bremer, Edwin

doi:10.3390/biomedicines10051175

Cited by 24 publications

(22 citation statements)

References 64 publications

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“…CD24 is highly expressed in multiple tumors and has, thus, been targeted in preclinical trials for lymphoma 65 , 69 , 73 , as well as lung, 14 , 74–76 colorectal, 75 , 77 , 78 bladder, 79 pancreatic, 14 , 74 ovarian, 14 , 74 , 80 liver, 75 , 81–83 breast, 84 and neuroendocrine 14 cancers in addition to osteosarcoma 85 and multiple myeloma 86 ( Table 3 ). Similar to CD20 targeting, the anti-CD24 mAb can bind directly and cluster CD24 to induce apoptosis, recruit NK cells via their Fc receptors to induce ADCC, induce complement-mediated cytotoxicity, as well as the recruitment of phagocytes to the tumor cells.…”

Section: Targeting Cd24 For Cancer Treatmentmentioning

confidence: 99%

“…62,63 In general, high CD24 expression has been associated with poor prognosis except in the case of multiple myeloma. [64][65][66][67][68][69][70] For chronic lymphocytic leukemia, high CD24 expression was associated with progressive vs stable disease. 71 Even though CD24 has been found to be expressed in most B cell malignancies to date, the protein expression levels do not always differentiate healthy from cancer patients due to high variability in expression.…”

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confidence: 99%

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CD24 as a Potential Therapeutic Target in Patients with B-Cell Leukemia and Lymphoma: Current Insights

Christian¹

2022

OTT

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CD24 is a highly glycosylated glycophosphatidylinositol (GPI)-anchored protein that is expressed in many types of differentiating cells and some mature cells of the immune system as well as the central nervous system. CD24 has been extensively used as a biomarker for developing B cells as its expression levels change over the course of B cell development. Functionally, engagement of CD24 induces apoptosis in developing B cells and restricts cell growth in more mature cell types. Interestingly, CD24 is also expressed on many hematological and solid tumors. As such, it has been investigated as a therapeutic target in many solid tumors including ovarian, colorectal, pancreatic, lung and others. Most of the B-cell leukemias and lymphomas studied to date express CD24 but its role as a therapeutic target in these malignancies has, thus far, been understudied. Here, I review what is known about CD24 biology with a focus on B cell development and activation followed by a brief overview of how CD24 is being targeted in solid tumors. This is followed by an assessment of the value of CD24 as a therapeutic target in B cell leukemia and lymphoma in humans, including an evaluation of the challenges in using CD24 as a target considering its pattern of expression on normal cells.

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Section: Targeting Cd24 For Cancer Treatmentmentioning

confidence: 99%

mentioning

confidence: 99%

CD24 as a Potential Therapeutic Target in Patients with B-Cell Leukemia and Lymphoma: Current Insights

Christian¹

2022

OTT

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“…CD24 mAb was found to increase macrophage phagocytosis [ 145 ], which suggests a potential immunotherapeutic target in MCL with the aim of improving innate immunity via disruption of the CD24/SIGLEC-10 axis. Another in vitro study found that CD24 mAb removed more than 90% of MCL cell lines [ 146 ]. Furthermore, CD24 mAb triggered phagocytosis in primary patient-derived MCL cells by autologous macrophages [ 146 ].…”

Section: Introductionmentioning

confidence: 99%

“…Another in vitro study found that CD24 mAb removed more than 90% of MCL cell lines [ 146 ]. Furthermore, CD24 mAb triggered phagocytosis in primary patient-derived MCL cells by autologous macrophages [ 146 ]. Treatment for in vitro MCL cell lines with CD24 mAb was superior to CD47 mAb, which suggests that CD24 mAb may be more effective in treating MCL than CD47 mAb [ 146 ].…”

Section: Introductionmentioning

confidence: 99%

“…Furthermore, CD24 mAb triggered phagocytosis in primary patient-derived MCL cells by autologous macrophages [ 146 ]. Treatment for in vitro MCL cell lines with CD24 mAb was superior to CD47 mAb, which suggests that CD24 mAb may be more effective in treating MCL than CD47 mAb [ 146 ]. Despite these studies, in vivo studies are also required to confirm these in vitro efficacies documented for MCL.…”

Section: Introductionmentioning

confidence: 99%

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Targeting macrophages in hematological malignancies: recent advances and future directions

Wang

Guo

et al. 2022

J Hematol Oncol

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Emerging evidence indicates that the detection and clearance of cancer cells via phagocytosis induced by innate immune checkpoints play significant roles in tumor-mediated immune escape. The most well-described innate immune checkpoints are the “don’t eat me” signals, including the CD47/signal regulatory protein α axis (SIRPα), PD-1/PD-L1 axis, CD24/SIGLEC-10 axis, and MHC-I/LILRB1 axis. Molecules have been developed to block these pathways and enhance the phagocytic activity against tumors. Several clinical studies have investigated the safety and efficacy of CD47 blockades, either alone or in combination with existing therapy in hematological malignancies, including myelodysplastic syndrome (MDS), acute myeloid leukemia (AML), and lymphoma. However, only a minority of patients have significant responses to these treatments alone. Combining CD47 blockades with other treatment modalities are in clinical studies, with early results suggesting a synergistic therapeutic effect. Targeting macrophages with bispecific antibodies are being explored in blood cancer therapy. Furthermore, reprogramming of pro-tumor macrophages to anti-tumor macrophages, and CAR macrophages (CAR-M) demonstrate anti-tumor activities. In this review, we elucidated distinct types of macrophage-targeted strategies in hematological malignancies, from preclinical experiments to clinical trials, and outlined potential therapeutic approaches being developed.

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Fucoidan‐Modified Au Nanocups With Tumor Targeting Inhibits CD24‐Mediated Immune Escape and Epithelial Mesenchymal Transition Through Precise Controlled Release of Anti‐CD24 Antibodies

Xie,

Jiang,

et al. 2024

Adv Funct Materials

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The presence of circulating tumor cells (CTCs) and inadequate immune response limit the therapy effectiveness of tumor metastasis. Epithelial‐mesenchymal transition (EMT), serving as the pivotal initial step in the formation of CTCs, plays a critical role in facilitating tumor metastasis. High expression of CD24 in tumor cells is strongly associated with EMT and immune evasion, but little work has been reported on the inhibitory effect of CD24 blockade on EMT. Here, a nanotherapeutic agent (Au/anti‐CD24@Fu) is fabricated through loading anti‐CD24 antibodies (anti‐CD24) onto Au nanocups, accompanied by surface modification with Fucoidan (Fu). Fu serves as a guide, while Au functions as a controller, jointly facilitating the precise delivery of anti‐CD24 to the tumor site and enabling controlled release. The synergistic collaboration between Fu and anti‐CD24 effectively eliminates the “don't eat me” signal mediated by CD24, thereby augmenting macrophage recognition and phagocytosis. Additionally, it simultaneously obstructs the EMT process facilitated by CD24‐P‐selectin from both ends, consequently impeding the formation of CTCs. Au/anti‐CD24@Fu displays favorable antitumor and anti‐metastasis effect in both 4T1‐bearing mice model and patient‐derived xenografts (PDX) model. This study validates the significance of CD24 blockade in augmenting the antitumor immune response and suppressing the EMT process.

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CD24 Is a Potential Immunotherapeutic Target for Mantle Cell Lymphoma

Cited by 24 publications

References 64 publications

CD24 as a Potential Therapeutic Target in Patients with B-Cell Leukemia and Lymphoma: Current Insights

CD24 as a Potential Therapeutic Target in Patients with B-Cell Leukemia and Lymphoma: Current Insights

Targeting macrophages in hematological malignancies: recent advances and future directions

Fucoidan‐Modified Au Nanocups With Tumor Targeting Inhibits CD24‐Mediated Immune Escape and Epithelial Mesenchymal Transition Through Precise Controlled Release of Anti‐CD24 Antibodies

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