ADAM17-mediated EGFR ligand shedding directs macrophage-promoted cancer cell invasion

Gnosa, Sebastian; Blasco, Laia Puig; Piotrowski, Krzysztof Bartłomiej; Freiberg, Marie L.; Savickas, Simonas; Madsen, Daniel H.; Keller, Ulrich auf dem; Kronqvist, Pauliina; Kveiborg, Marie

doi:10.1172/jci.insight.155296

Cited by 13 publications

(15 citation statements)

References 77 publications

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“…ADAM17-mediated JAM-A/ FIIR shedding is responsible for aging-related abnormal endothelial remodeling (156). However, other substrates, like EGFR ligands (17,97,180), E-cadherin (124), VLDLR (4), IL-11R (5), CD137 (94), P75 (11), GPIBa (6), HPP1 (119), and NRG1 (10) are precursor proteins or fusion proteins that can yield active components or soluble active receptors only after cleavage and release by ADAM17 (Figure 2). Evidence suggests that ADAM17 promotes tumor-associated macrophage polarization and angiotensin II-mediated pro-growth and promigration signals by shedding EGFR ligands, including heparinbinding EGF-like growth factor (HB-EGF) and AREG (members of the EGF family), from the cell membrane (17,32).…”

Section: Adam17 Mediates Substrate Shedding Activitymentioning

confidence: 99%

“…Our previous study showed that the expression of ADAM17 was associated with infiltration of multiple immune cells, including macrophages (20), in TCGA pan-cancer samples and yet the specific regulatory mechanism of ADAM17 is unknown. Recently, Gnosa et al have revealed the positive roles of ADAM17 in regulating the polarization of TAMs (17). By using bioinformatics analysis based on the TCGA dataset and immunohistochemical analysis from triple-negative breast cancer cohort, the authors first confirmed that highly expressed ADAM17 in tumors is positively correlated with tumorigenic macrophage markers CD163 or CD206.…”

Section: Regulation Of Macrophages By Adam17mentioning

confidence: 99%

“…More importantly, ADAM17 is contributory to the occurrence and development of cancers, including lung carcinoma (10), ovarian carcinoma (11), breast carcinoma (12)(13)(14), gastric carcinoma (15), and cervical carcinoma (16). Interestingly, it regulates some immune signaling pathways through the shedding activity, which may facilitate the inflammatory response in tumor development (17)(18)(19). However, the study of the relationship between the abnormal expression of this metalloproteinase in tumors and its immune regulation is still not well studied.…”

Section: Introductionmentioning

confidence: 99%

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Immunomodulatory role of metalloproteinase ADAM17 in tumor development

et al. 2022

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ADAM17 is a member of the a disintegrin and metalloproteinase (ADAM) family of transmembrane proteases involved in the shedding of some cell membrane proteins and regulating various signaling pathways. More than 90 substrates are regulated by ADAM17, some of which are closely relevant to tumor formation and development. Besides, ADAM17 is also responsible for immune regulation and its substrate-mediated signal transduction. Recently, ADAM17 has been considered as a major target for the treatment of tumors and yet its immunomodulatory roles and mechanisms remain unclear. In this paper, we summarized the recent understanding of structure and several regulatory roles of ADAM17. Importantly, we highlighted the immunomodulatory roles of ADAM17 in tumor development, as well as small molecule inhibitors and monoclonal antibodies targeting ADAM17.

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Section: Adam17 Mediates Substrate Shedding Activitymentioning

confidence: 99%

Section: Regulation Of Macrophages By Adam17mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Immunomodulatory role of metalloproteinase ADAM17 in tumor development

et al. 2022

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“…Our results suggest that it might be possible to screen for molecules that selectively affect the orientation or presentation of the cleavage site(s) of EGFR ligands and other substrate proteins to ADAM17/iR2. This could help block the activity of EGFR ligands implicated in cancer and inflammation (e.g., AREG, EREG, [ 48 , 49 , 50 , 51 , 52 ]) without affecting the function of TGFα in protection of the skin and intestinal barrier [ 13 , 16 , 17 ]. This, in turn, could provide novel treatment options for diseases that depend on the dysregulated processing of specific EGFR ligands.…”

Section: Discussionmentioning

confidence: 99%

Identification of Molecular Determinants in iRhoms1 and 2 That Contribute to the Substrate Selectivity of Stimulated ADAM17

Zhao

Dávila

et al. 2022

IJMS

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The metalloprotease ADAM17 is a key regulator of the TNFα, IL-6R and EGFR signaling pathways. The maturation and function of ADAM17 is controlled by the seven-membrane-spanning proteins iRhoms1 and 2. The functional properties of the ADAM17/iRhom1 and ADAM17/iRhom2 complexes differ, in that stimulated shedding of most ADAM17 substrates tested to date can be supported by iRhom2, whereas iRhom1 can only support stimulated shedding of very few ADAM17 substrates, such as TGFα. The first transmembrane domain (TMD1) of iRhom2 and the sole TMD of ADAM17 are important for the stimulated shedding of ADAM17 substrates by iRhom2. However, little is currently known about how the iRhoms interact with different substrates to control their stimulated shedding by ADAM17. To provide new insights into this topic, we tested how various chimeras between iRhom1 and iRhom2 affect the stimulated processing of the EGFR-ligands TGFα (iRhom1- or 2-dependent) and EREG (iRhom2-selective) by ADAM17. This uncovered an important role for the TMD7 of the iRhoms in determining their substrate selectivity. Computational methods utilized to characterize the iRhom1/2/substrate interactions suggest that the substrate selectivity is determined, at least in part, by a distinct accessibility of the substrate cleavage site to stimulated ADAM17. These studies not only provide new insights into why the substrate selectivity of stimulated iRhom2/ADAM17 differs from that of iRhom1/ADAM17, but also suggest new approaches for targeting the release of specific ADAM17 substrates.

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“…The protumorigenic role of ADAMs has been further confirmed in vitro and in murine cancer models, where studies have shown a role in supporting tumor growth and metastasis 15‐17 . Although the implication of ADAMs in cell‐ECM and cell‐cell interactions has been shown in vitro, 18,19 their role in the crosstalk between cancer cells and the TME in murine cancer models is scarcely explored 20‐22 …”

Section: Introductionmentioning

confidence: 99%

Loss of cancer cell‐derived ADAM15 alters the tumor microenvironment in colorectal tumors

Puig‐Blasco,

Piotrowski,

Michaelsen

et al. 2023

Intl Journal of Cancer

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Tumor progression and response to treatment are highly affected by interactions between cancer cells and the tumor microenvironment (TME). Many of the soluble factors and signaling receptors involved in this crosstalk are shed by a disintegrin and metalloproteinases (ADAMs). Upregulation of ADAM15 has been linked to worse survival in cancer patients and a tumor‐promoting function both in vitro and in murine cancer models. Although ADAM15 has been involved in cell‐cell and cell‐extracellular matrix interactions, its role in the crosstalk between cancer cells and the TME in vivo remains unexplored. Therefore, we aimed to understand how ADAM15 regulates the cell composition of the TME and how it affects tumor progression. Here, we showed an upregulation of ADAM15 in tumor tissues from rectal cancer patients. Subcutaneous injection of wildtype and ADAM15‐knockout CT26 colon cancer cells in syngeneic mice confirmed the protumorigenic role of ADAM15. Profiling of tumors revealed higher immune cell infiltration and cancer cell apoptosis in the ADAM15‐deficient tumors. Specifically, loss of ADAM15 led to a reduced number of granulocytes and higher infiltration of antigen‐presenting cells, including dendritic cells and macrophages, as well as more T cells. Using in vitro assays, we confirmed the regulatory effect of ADAM15 on macrophage migration and identified ADAM15‐derived CYR61 as a potential molecular mediator of this effect. Based on these findings, we speculate that targeting ADAM15 could increase the infiltration of immune cells in colorectal tumors, which is a prerequisite for effective immunotherapy.

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ADAM17-mediated EGFR ligand shedding directs macrophage-promoted cancer cell invasion

Cited by 13 publications

References 77 publications

Immunomodulatory role of metalloproteinase ADAM17 in tumor development

Immunomodulatory role of metalloproteinase ADAM17 in tumor development

Identification of Molecular Determinants in iRhoms1 and 2 That Contribute to the Substrate Selectivity of Stimulated ADAM17

Loss of cancer cell‐derived ADAM15 alters the tumor microenvironment in colorectal tumors

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