A novel immunotherapy targeting MMP-14 limits hypoxia, immune suppression and metastasis in triple-negative breast cancer models

Ling, Binbing; Watt, Kathleen; Banerjee, Sunandan; Newsted, Daniel; Truesdell, Peter; Adams, Jarrett; Sidhu, Sachdev S.; Craig, Andrew W.B.

doi:10.18632/oncotarget.17702

Cited by 72 publications

(54 citation statements)

References 36 publications

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“…However, the high similarity of protein folding and catalytic chemistry among MMP family members presents a daunting challenge for the generation of highly selective compound inhibitors (Turk, ). Our studies (Lopez, Nam, Kaihara, Mustafa & Ge, ; Nam, Fang, Rodriguez, Lopez, & Ge, ; Nam, Rodriguez, Remacle, Strongin, & Ge, ), among others (Appleby et al, ; Devy et al, ; Ling et al, ; Udi et al, ), demonstrated the feasibility that antibody‐based inhibitors could exhibit the desired high selectivity. Particularly, Fab3A2 with 4.8 nM affinity, 9.7 nM potency, and high selectivity toward MMP‐14 was isolated from a library containing ultralong CDR H3s (Nam et al, ).…”

Section: Introductionmentioning

confidence: 61%

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Epitope‐specific affinity maturation improved stability of potent protease inhibitory antibodies

Lopez

Chen

Ramirez

et al. 2018

Biotech & Bioengineering

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Targeting effectual epitopes is essential for therapeutic antibodies to accomplish their desired biological functions. This study developed a competitive dual color fluorescence-activated cell sorting (FACS) to maturate a matrix metalloprotease 14 (MMP-14) inhibitory antibody. Epitope-specific screening was achieved by selection on MMP-14 during competition with N-terminal domain of tissue inhibitor of metalloproteinase-2 (TIMP-2) (nTIMP-2), a native inhibitor of MMP-14 binding strongly to its catalytic cleft. 3A2 variants with high potency, selectivity, and improved affinity and proteolytic stability were isolated from a random mutagenesis library. Binding kinetics indicated that the affinity improvements were mainly from slower dissociation rates. In vitro degradation tests suggested the isolated variants had half lives 6-11-fold longer than the wt. Inhibition kinetics suggested they were competitive inhibitors which showed excellent selectivity toward MMP-14 over highly homologous MMP-9. Alanine scanning revealed that they bound to the vicinity of MMP-14 catalytic cleft especially residues F204 and F260, suggesting that the desired epitope was maintained during maturation. When converted to immunoglobulin G, B3 showed 5.0 nM binding affinity and 6.5 nM inhibition potency with in vivo half-life of 4.6 days in mice. In addition to protease inhibitory antibodies, the competitive FACS described here can be applied for discovery and engineering biosimilars, and in general for other circumstances where epitope-specific modulation is needed.

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Section: Introductionmentioning

confidence: 61%

“…Our studies (Lopez, Nam, Kaihara, Mustafa & Ge, 2017;Nam, Fang, Rodriguez, Lopez, & Ge, 2017;Nam, Rodriguez, Remacle, Strongin, & Ge, 2016), among others (Appleby et al, 2017;Devy et al, 2009;Ling et al, 2017;Udi et al, 2015), demonstrated the feasibility that antibody-based inhibitors could exhibit the desired high selectivity.…”

mentioning

confidence: 65%

Epitope‐specific affinity maturation improved stability of potent protease inhibitory antibodies

Lopez

Chen

Ramirez

et al. 2018

Biotech & Bioengineering

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“…However, gelatin is a substrate for multiple proteases, and MMPs were expressed on the surface of yeast cells (Diehl et al, 2011), which are quite different from mammalian cell surfaces. As several selective and/or secondary binding site (exosite) MT1-MMP inhibitors have been described (Levin, Udi, Solomonov, & Sagi, 2017;Ling et al, 2017;Pahwa et al, 2014;Santamaria & de Groot, 2018), the evaluation of activity at the cell surface will allow for examination of such inhibitors in a more native-like environment. This will also facilitate the development of inhibitors that may act indirectly on MT1-MMP activity.…”

Section: Discussionmentioning

confidence: 99%

Characterization and regulation of MT1‐MMP cell surface‐associated activity

et al. 2018

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Quantitative assessment of MT1‐MMP cell surface‐associated proteolytic activity remains undefined. Presently, MT1‐MMP was stably expressed and a cell‐based FRET assay developed to quantify activity toward synthetic collagen‐model triple‐helices. To estimate the importance of cell surface localization and specific structural domains on MT1‐MMP proteolysis, activity measurements were performed using a series of membrane‐anchored MT1‐MMP mutants and compared directly with those of soluble MT1‐MMP. MT1‐MMP activity (kcat/KM) on the cell surface was 4.8‐fold lower compared with soluble MT1‐MMP, with the effect largely manifested in kcat. Deletion of the MT1‐MMP cytoplasmic tail enhanced cell surface activity, with both kcat and KM values affected, while deletion of the hemopexin‐like domain negatively impacted KM and increased kcat. Overall, cell surface localization of MT1‐MMP restricts substrate binding and protein‐coupled motions (based on changes in both kcat and KM) for catalysis. Comparison of soluble and cell surface‐bound MT2‐MMP revealed 12.9‐fold lower activity on the cell surface. The cell‐based assay was utilized for small molecule and triple‐helical transition state analog MMP inhibitors, which were found to function similarly in solution and at the cell surface. These studies provide the first quantitative assessments of MT1‐MMP activity and inhibition in the native cellular environment of the enzyme.

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“…Other inhibitory molecules include Fab R2C7 which is highly selective for MMP‐14 (Lopez, Nam, Kaihara, Mustafa, & Ge, ). Another MMP‐14 inhibitor that inhibits the catalytic domain of MMP‐14, Fab 3369, prevents the ECM degradation by MMP‐14 invasion of MDA‐MB‐231 cells (Ling et al, ). The blockade of MMP‐14 has been shown to overcome the immunosuppressive TME in metastatic cases BC (Li et al, ).…”

Section: Immune Checkpoint Inhibitors (Icis)mentioning

confidence: 99%

“…One of the MMP family members, MMP-14 can degrade collagen, which is required for invadopodia formation (Leong et al, 2014). Targeting the metastasis early events for example the degradation step of ECM and the cancer cells invasion, may proved beneficial effects in TNBC (Ling et al, 2017).…”

Section: Icis Combined With Anti-mmp-14mentioning

confidence: 99%

Single peptides and combination modalities for triple negative breast cancer

Razazan

Behravan

2019

Journal Cellular Physiology

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Unlike other types of breast cancers (BCs), no specific therapeutic targets have been established for triple negative breast cancer (TNBC). Therefore, chemotherapy and radiotherapy are the only available adjuvant therapeutic choices for TNBC. New emerging reports show that TNBC is associated with higher numbers of intratumoral tumor infiltrating lymphocytes. This is indicative of host anti-TNBC immune surveillance and suggesting that immunotherapy can be considered as a therapeutic approach for TNBC management. Recent progress in molecular mechanisms of tumor-immune system interaction and cancer vaccine development studies, fast discoveries and FDA approvals of immune checkpoint inhibitors, chimeric antigen receptor T-cells, and oncolytic virotherapy have significantly attracted attention and research directions toward the immunotherapeutic approach to TNBC. Here in this review different aspects of TNBC immunotherapies including the host immune system-tumor interactions, the tumor microenvironment, the relevant molecular targets for immunotherapy, and clinical trials in the field are discussed.

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A novel immunotherapy targeting MMP-14 limits hypoxia, immune suppression and metastasis in triple-negative breast cancer models

Cited by 72 publications

References 36 publications

Epitope‐specific affinity maturation improved stability of potent protease inhibitory antibodies

Epitope‐specific affinity maturation improved stability of potent protease inhibitory antibodies

Characterization and regulation of MT1‐MMP cell surface‐associated activity

Single peptides and combination modalities for triple negative breast cancer

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