B cells inhibit the antitumor immunity against an established murine fibrosarcoma

Maglioco, Andrea; Machuca, Damián; Badano, María Noel; Nannini, Paula Romina; Camerano, Gabriela; Costa, Héctor; Meiss, Roberto P.; Ruggiero, Raúl A.; Giordano, Mirta; Dran, Graciela

doi:10.3892/ol.2017.5810

Cited by 10 publications

(14 citation statements)

References 35 publications

(63 reference statements)

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“…B cells rapidly expand in response to tumor challenge and up-regulate immunoglobulin-related genes in TDLNs relative to NDLNs (19,105,106); however, the effects of antibodies on tumor progression seem to vary widely based on tumor model, anatomical location, and timing. Tumor-binding immunoglobulin G (IgG) antibodies can accumulate in tumors where they are taken up by DCs to initiate cytotoxic T cell-mediated tumor clearance (107), and B cell depletion before tumor inoculation actually accelerates primary tumor growth (108). However, when B cells are depleted in established tumor-bearing mice, IFN-producing CD8 + T cells accumulate in TDLNs and lead to improved tumor control (108).…”

Section: B Cells and Tumor-binding Antibodiesmentioning

confidence: 99%

“…Tumor-binding immunoglobulin G (IgG) antibodies can accumulate in tumors where they are taken up by DCs to initiate cytotoxic T cell-mediated tumor clearance (107), and B cell depletion before tumor inoculation actually accelerates primary tumor growth (108). However, when B cells are depleted in established tumor-bearing mice, IFN-producing CD8 + T cells accumulate in TDLNs and lead to improved tumor control (108). These findings suggest that B cells may be protective but undergo a tumor-dependent shift in function that can support tumor progression in TDLNs.…”

Section: B Cells and Tumor-binding Antibodiesmentioning

confidence: 99%

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Tumor-draining lymph nodes: At the crossroads of metastasis and immunity

2021

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Early engagement of the lymphatic system by solid tumors in peripheral, nonlymphoid tissues is a clinical hallmark of cancer and often forecasts poor prognosis. The significance of lymph node metastasis for distant spread, however, has been questioned by large-scale lymph node dissection trials and the likely prevalence of direct hematogenous metastasis. Still, an emerging appreciation for the immunological role of the tumor-draining lymph node has renewed interest in its basic biology, role in metastatic progression, antitumor immunity, and patient outcomes. In this review, we discuss our current understanding of the early mechanisms through which tumors engage lymphatic transport and condition tumor-draining lymph nodes, the significance of these changes for both metastasis and immunity, and potential implications of the tumor-draining lymph node for immunotherapy.

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Section: B Cells and Tumor-binding Antibodiesmentioning

confidence: 99%

Section: B Cells and Tumor-binding Antibodiesmentioning

confidence: 99%

Tumor-draining lymph nodes: At the crossroads of metastasis and immunity

2021

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“…Во-первых, это формирование, активация и перераспределение (миграция) в организме всех клеток иммунной системы, участвующих в инициации и развитии противоопухолевого иммунитета [5,7,28]. И, во-вторых, развитие «защитной» реакции со стороны опухоли, реализующейся в изменении антигенной структуры малигнизированных клеток, синтезом различных цитокинов и других биологически активных веществ, что приводит к ингибированию противоопухолевого иммунитета на различных этапах развития иммунной реакции [1,20,33 [3,11,27]. Однако в ряде работ отмечается, что генерация ДК из моноцитов периферической крови осуществляется недостаточно эффективно: формируются ДК со сниженными функциональными свойствами.…”

Section: Discussionunclassified

“…Функциональная активность ДК, дифференцированных из моноцитов периферической крови, может во многом зависеть от функционального состояния самих моноцитов и от эффекторных и регуляторных процессов в иммунной системе, которые формируются в процессе развития иммуноопосредованных заболеваний. Доказано, что развитие опухоли в организме обусловливает ингибирование противоопухолевого иммунитета, которое реализуется через нарушение соотношения эффекторных и регуляторных субпопуляций Т-лимфоцитов, синтеза супрессирующих цитокинов и снижение активности эффекторных реакций [1,20,32]. Ранее нами установлено, что у больных раком почки (РП) в периферической крови повышается количество CD14 low CD16 + моноцитов, выявляется дисбаланс в экспрессии активационных маркеров и снижается интенсивность респираторного взрыва [4].…”

Section: Introductionunclassified

Phenotypic Peculiarities of Dendritiс Cells Differentiated From Blood Monocytes in Patients With Kidney Cancer

Савченко¹,

Борисов²,

Kudryavtsev³

et al. 2018

Med. immunol.

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Савченко А.А. и др. Medical Immunology (Russia)/Meditsinskaya Immunologiya Медицинская Иммунология вых людей и больных РП выравнивается, но при РП меньше формируется аДК с высокоактивным фенотипом (CD83 + CD80 high CD86 high и CD83 + CD80 high CD86 high HLA-DR +). Более того, при онкологии аДК с фенотипом CD83 + CD80 high CD86 high слабее экспрессируют рецепторы для проявления костимуляторной и антигенпрезентирующей активности. Различия в фенотипе нДК и аДК у здоровых людей и больных РП могут определяться различиями в фенотипе и функциональной активности моноцитов крови и иммунодепрессивными факторами, синтезируемые опухолью.

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“…B cell-deficient mice inhibit tumor growth through increased cytotoxic CD8 T cell and reduced regulatory T cell populations in several tumor models, such as EL4 thymoma, MC38 colon carcinoma, and EMT-6 breast carcinoma ( Shah et al, 2005 ; Tadmor et al, 2011 ; Zhang et al, 2013 ). In a fibrosarcoma model, depleting B cells before tumor implantation accelerates tumor growth while depleting B cells after tumor establishment suppresses tumor growth, suggesting that B cells may contribute to pro-tumor or anti-tumor immunity depending on the stage of tumor growth ( Maglioco et al, 2017 ).…”

Section: Introductionmentioning

confidence: 99%

Tumor-Draining Lymph Node Reconstruction Promotes B Cell Activation During E0771 Mouse Breast Cancer Growth

Louie

Leung

et al. 2022

Front. Pharmacol.

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Lymph node metastasis is associated with tumor aggressiveness and poor prognosis in patients. Despite its significance in cancer progression, how immune cells in the tumor-draining lymph node (TDLN) participate in cancer immune regulation remains poorly understood. It has been reported that both anti-tumor and exhausted tumor-specific T cells can be induced in the TDLNs; however, B cell activation and maturation in the TDLN has received far less attention. In our studies using C57BL/6 mouse syngeneic E0771 breast cancer or B16F10 melanoma cell lines, tumor-associated antigens were found colocalized with the follicular dendritic cells (FDCs) in the germinal centers (GCs), where antigen-specific B cell maturation occurs. LN conduits and the subcapsular sinus (SCS) macrophages are two major routes of antigen trafficking to FDCs. Tumor growth induced LN conduit expansion in the B cell zone and disrupted the SCS macrophage layer, facilitating both the entry of tumor-associated antigens into the B cell zone and access to FDCs located in the GCs. Regional delivery of clodronate liposome specifically depleted SCS macrophages in the TDLN, increasing GC formation, and promoting tumor growth. Our study suggests that TDLN reconstruction creates a niche that favors B cell activation and maturation during tumor growth.

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B cells inhibit the antitumor immunity against an established murine fibrosarcoma

Cited by 10 publications

References 35 publications

Tumor-draining lymph nodes: At the crossroads of metastasis and immunity

Tumor-draining lymph nodes: At the crossroads of metastasis and immunity

Phenotypic Peculiarities of Dendritiс Cells Differentiated From Blood Monocytes in Patients With Kidney Cancer

Tumor-Draining Lymph Node Reconstruction Promotes B Cell Activation During E0771 Mouse Breast Cancer Growth

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