Tumor-Associated Lymphatic Vessels Upregulate PDL1 to Inhibit T-Cell Activation

Dieterich, Lothar C.; Ikenberg, Kristian; Cetintas, Timur; Kapaklikaya, Kübra; Hutmacher, Cornelia; Detmar, Michael

doi:10.3389/fimmu.2017.00066

Cited by 110 publications

(105 citation statements)

References 35 publications

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“…Our results are striking in terms of the strong inflammatory gene expression signature of 4T1‐associated LECs, which included induction of many chemokines and adhesion molecules. We also found a trend (log 2 FC = 1.96, FDR = 0.68) toward increased expression of the T cell inhibitory protein PD‐L1, which is in line with our own previous observations . Clearly, this proinflammatory gene expression signature is likely to have a plethora of effects on tumor progression, metastasis and host immunity.…”

Section: Discussionsupporting

confidence: 91%

“…Cell suspensions of control skin, 4T1 tumors and tumor‐draining LNs were prepared as described . For staining, the following antibodies were used: CD45‐APC/Cy7 or CD45‐PacificBlue (Biolegend 103116, 103126), CD31‐APC (BD 551262), podoplanin‐PE (eBioscience, San Diego, CA, 12‐5381‐82), CD3‐PE/Cy7 (Biolegend 100220), CD11b‐BV605 (Biolegend 101257), Ly6C‐PE (Biolegend 128008), Ly6G‐FITC (Biolegend 127606), F4/80‐Alexa647 (BioRad MCA497G), VE‐cadherin‐APC (Biolegend 138012) and goat antimouse VCAM‐1 (R&D AF643), followed by washing and labeling with a secondary donkey antigoat‐Alexa488 antibody.…”

Section: Methodsmentioning

confidence: 99%

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Transcriptional profiling of breast cancer‐associated lymphatic vessels reveals VCAM‐1 as regulator of lymphatic invasion and permeability

Kapaklikaya

Cetintas

Proulx

et al. 2019

Intl Journal of Cancer

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Tumor‐associated lymphangiogenesis and lymphatic invasion of tumor cells correlate with poor outcome in many tumor types, including breast cancer. Various explanations for this correlation have been suggested in the past, including the promotion of lymphatic metastasis and an immune‐inhibitory function of lymphatic endothelial cells (LECs). However, the molecular features of tumor‐associated lymphatic vessels and their implications for tumor progression have been poorly characterized. Here, we report the first transcriptional analysis of tumor‐associated LECs directly isolated from the primary tumor in an orthotopic mouse model of triple negative breast cancer (4T1). Gene expression analysis showed a strong upregulation of inflammation‐associated genes, including endothelial adhesion molecules such as VCAM‐1, in comparison to LECs derived from control tissue. In vitro experiments demonstrated that VCAM‐1 is not involved in the adhesion of tumor cells to LECs but unexpectedly promoted lymphatic permeability by weakening of lymphatic junctions, most likely through a mechanism triggered by interactions with integrin α4 which was also induced in tumor‐associated LECs. In line with this, in vivo blockade of VCAM‐1 reduced lymphatic invasion of 4T1 cells. Taken together, our findings suggest that disruption of lymphatic junctions and increased permeability via tumor‐induced lymphatic VCAM‐1 expression may represent a new target to block lymphatic invasion and metastasis.

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Section: Discussionsupporting

confidence: 91%

Section: Methodsmentioning

confidence: 99%

Transcriptional profiling of breast cancer‐associated lymphatic vessels reveals VCAM‐1 as regulator of lymphatic invasion and permeability

Kapaklikaya

Cetintas

Proulx

et al. 2019

Intl Journal of Cancer

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“…In a murine model of lymphatic-enriched melanoma, we have found that VEGF-Cstimulated LECs in the tdLNs tolerize antitumor CD8 + T cells through cross-presentation of tumor Ags [182]. Very recently, PD-L1 expression by LECs was shown to have a crucial role in the inhibition of CD8 + T cell response in the context of tumor [220]. These studies underline the ability of LECs to extend their Ag presentation abilities beyond PTAs, therefore broadening their role as an active player in immune responses.…”

Section: Antigen Presentation To Cd8 + T Cellsmentioning

confidence: 99%

Exploiting lymphatic vessels for immunomodulation: Rationale, opportunities, and challenges

Maisel

Sasso

Potin

et al. 2017

Advanced Drug Delivery Reviews

102

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Lymphatic vessels are the primary route of communication from peripheral tissues to the immune system; as such, they represent an important component of local immunity. In addition to their transport functions, new immunomodulatory roles for lymphatic vessels and lymphatic endothelial cells have come to light in recent years, demonstrating that lymphatic vessels help shape immune responses in a variety of ways: promoting tolerance to self-antigens, archiving antigen for later presentation, dampening effector immune responses, and resolving inflammation, among others. In addition to these new biological insights, the growing field of immunoengineering has begun to explore therapeutic approaches to utilize or exploit the lymphatic system for immunotherapy.

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“…An increase in VEGF‐C expression in tumors is highly correlated with LN metastasis and poor prognosis in individuals with different tumor types, including skin, breast and lung cancers . Furthermore, LEC not only present antigens and modulate immune cell activation in physiology conditions but also promote tumor progression and metastasis by inhibiting the function of immune cells (Figure ) . Mechanistically, VEGF‐C plays an immunosuppressive role for LEC to scavenge and cross‐present antigens for direct suppression of cytotoxic T lymphocytes .…”

Section: Functional Heterogeneity Of Tumor Lymphangiogenesismentioning

confidence: 99%

“…2 Furthermore, LEC not only present antigens and modulate immune cell activation in physiology conditions 64,65 but also promote tumor progression and metastasis by inhibiting the function of immune cells (Figure 3). 40,66 Mechanistically, VEGF-C plays an immunosuppressive role for LEC to scavenge and cross-present antigens for direct suppression of cytotoxic T lymphocytes. 61 LEC can also express immunosuppressive factors such as TGF-β and nitric oxide to maintain peripheral tolerance to self-antigens in lymph nodes by directly or indirectly regulating T-cell fate and function in immunity.…”

Section: Paradoxical Roles In Antitumor Immune Responsementioning

confidence: 99%

Heterogeneity of tumor lymphangiogenesis: Progress and prospects

Luo

2018

Cancer Science

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Lymphangiogenesis and increased expression of lymphangiogenic growth factors are associated with high rates of lymph node (LN) metastasis and with poor prognosis in some, but not all, solid tumors. In addition to its involvement in metastasis, lymphangiogenesis has been shown to have other roles in tumor pathogenesis, such as the niche function of tumor stem cells and regulatory functions of antitumor immune responses. In contrast, evidence has accumulated that tumor‐induced lymphangiogenesis displays the heterogeneity in gene signature, structure, cellular origins and functional plasticity. This review summarizes the advances in the research on the heterogeneity of tumor lymphangiogenesis and discusses how it may contribute to functional complexity and multiplicity of lymphangiogenesis in tumor progression.

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Tumor-Associated Lymphatic Vessels Upregulate PDL1 to Inhibit T-Cell Activation

Cited by 110 publications

References 35 publications

Transcriptional profiling of breast cancer‐associated lymphatic vessels reveals VCAM‐1 as regulator of lymphatic invasion and permeability

Transcriptional profiling of breast cancer‐associated lymphatic vessels reveals VCAM‐1 as regulator of lymphatic invasion and permeability

Exploiting lymphatic vessels for immunomodulation: Rationale, opportunities, and challenges

Heterogeneity of tumor lymphangiogenesis: Progress and prospects

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