Midkine rewires the melanoma microenvironment toward a tolerogenic and immune-resistant state

Cerezo-Wallis, Daniela; Contreras-Alcalde, Marta; Troulé, Kevin; Catena, Xavier; Mucientes, Cynthia; Calvo, Tonantzin G.; Cañón, Estela; Tejedo, Cristina; Pennacchi, Paula Comune; Hogan, Sabrina A.; Kölblinger, Peter; Tejero, Héctor; Chen, Andrew X.; Ibarz, Nuria; Graña‐Castro, Osvaldo; Martínez, Lola; Muñoz, Javier; Ortiz‐Romero, Pablo L.; Rodríguez‐Peralto, José Luis; Gómez‐López, Gonzalo; Al‐Shahrour, Fátima; Rabadán, Raúl; Levesque, Mitchell P.; Olmeda, David; Soengas, María S.

doi:10.1038/s41591-020-1073-3

Cited by 84 publications

(99 citation statements)

References 66 publications

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“…Treatment with BO‐110 started when the cutaneous lesions were palpable (around 100 mm 3 ; see arrows for all panels in Fig 6 ) and proceeded for 2 weeks. In the absence of BO‐110, both of these lines are very aggressive as previously reported (Olmeda et al , 2017 ; Cerezo‐Wallis et al , 2020 ). In these conditions, Vegfr3 Luc emission correlated with tumor growth at the site of implantation (Fig 6B and J ), and was induced systemically in the lymph nodes (Fig 6C and K ), spleen (Fig 6D and L ), lung (Fig 6F and M ), and liver (Fig 6E and N ).…”

Section: Resultssupporting

confidence: 81%

“…In particular, our findings revealing circulating MDK as a biomarker that reflects reduced tumor burden after BO‐110 treatment may prove useful to assess the antitumoral activity of this compound beyond less specific IFN‐associated markers. Importantly, we have recently reported that MDK exerts potent immune‐suppressive roles on macrophages and cytotoxic T cells (Cerezo‐Wallis et al , 2020 ). Therefore, pharmacological blockade of MDK may have the added value of not only interfering with tumor neolymphangiogenesis and metastasis, but also impinging on the immune milieu.…”

Section: Discussionmentioning

confidence: 99%

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Live imaging of neolymphangiogenesis identifies acute antimetastatic roles of dsRNA mimics

et al. 2021

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Long-range communication between tumor cells and the lymphatic vasculature defines competency for metastasis in different cancer types, particularly in melanoma. Nevertheless, the discovery of selective blockers of lymphovascular niches has been compromised by the paucity of experimental systems for whole-body analyses of tumor progression. Here, we exploit immunocompetent and immunodeficient mouse models for live imaging of Vegfr3driven neolymphangiogenesis, as a versatile platform for drug screening in vivo. Spatiotemporal analyses of autochthonous melanomas and patient-derived xenografts identified double-stranded RNA mimics (dsRNA nanoplexes) as potent inhibitors of neolymphangiogenesis, metastasis, and post-surgical disease relapse. Mechanistically, dsRNA nanoplexes were found to exert a rapid dual action in tumor cells and in their associated lymphatic vasculature, involving the transcriptional repression of the lymphatic drivers Midkine and Vegfr3, respectively. This suppressive function was mediated by a cell-autonomous type I interferon signaling and was not shared by FDA-approved antimelanoma treatments. These results reveal an alternative strategy for targeting the tumor celllymphatic crosstalk and underscore the power of Vegfr3lymphoreporters for pharmacological testing in otherwise aggressive cancers.

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Section: Resultssupporting

confidence: 81%

Section: Discussionmentioning

confidence: 99%

Live imaging of neolymphangiogenesis identifies acute antimetastatic roles of dsRNA mimics

et al. 2021

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“…As expected, EGLN3 inactivation attenuated interleukin 4-induced M2 polarization, as indicated by decreased mRNA and protein expression of arginase (Arg) 1 (Fig. 5N, O), a marker of M2 macrophages [37]. Albeit to a less extent, EGLN3 inactivation promoted M1 polarization of macrophages, as judged by the expression of inducible nitric oxide synthase (iNOS) (Fig.…”

Section: Genetic Inactivation Of Egln3 Hydroxylase Inhibits Macrophag...supporting

confidence: 64%

Inactivation of EGLN3 hydroxylase facilitates Erk3 degradation via autophagy and impedes lung cancer growth

et al. 2022

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EGLN3 is critically important for growth of various cancers including lung cancer. However, virtually nothing is known about the role and mechanism for EGLN3 hydroxylase activity in cancers. EGLN3 catalyzes the hydroxylation of extracellular signal-regulated kinase 3 (Erk3), a potent driver of cancers. The role and mechanism for EGLN3-induced stabilization of Erk3 remain to be defined. Here, we show that Erk3 interacts with heat shock cognate protein of 70 kDa (HSC70) and lysosome-associated membrane protein type 2 A (LAMP2A), two core components of chaperone-mediated autophagy (CMA). As a consequence, Erk3 is degraded by the CMA-lysosome pathway. EGLN3-catalyzed hydroxylation antagonizes CMA-dependent destruction of Erk3. Mechanistically, hydroxylation blunts the interaction of Erk3 with LAMP2A, thereby blocking lysosomal decay of Erk3. EGLN3 inactivation inhibits macrophage migration, efferocytosis, and M2 polarization. Studies using EGLN3 catalytically inactive knock-in mice indicate that inactivation of EGLN3 hydroxylase in host cells ameliorates LLC cancer growth through reprogramming the tumor microenvironment (TME). Adoptive transfer of macrophages with inactivated EGLN3 restrains tumor growth by mounting anti-tumor immunity and restricting angiogenesis. Administration of EGLN3 hydroxylase pharmacologic inhibitor to mice bearing LLC carcinoma impedes cancer growth by targeting the TME. LLC cells harboring inactivated EGLN3 exhibit reduced tumor burden via mitigating immunosuppressive milieu and inducing cancer senescence. This study provides novel insights into the role of CMA in regulating Erk3 stability and the mechanism behind EGLN3-enhanced stability of Erk3. This work demonstrates that inactivation of EGLN3 in malignant and stromal cells suppresses tumor by orchestrating reciprocal interplays between cancer cells and the TME. This work sheds new light on the role and mechanism for EGLN3 catalytic activity in regulating cancer growth. Manipulating EGLN3 activity holds promise for cancer treatment.

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“…Serum midkine levels in healthy subjects are mostly determined within a narrow range that depends on the applied detection system. Beyond these "background" levels, several diseases are known to be accompanied by elevated midkine serum levels, e.g., cancers of different origin, ischemia of brain, limbs or kidneys [33], and congestive heart failure [4,[34][35][36][37].…”

Section: Discussionmentioning

confidence: 99%

“…Midkine received its designation as a heparin binding factor, which was initially described as an embryonic growth factor with strong expression during mid-gestation and within kidneys. Pleiotropic functions have been identified beyond pregnancy, involving cellular survival programs, chemotaxis of neutrophils [1], and propagation of neoangiogenesis [2][3][4]. The potency of this specific growth factor is illustrated in experimental animal models with genetic ablation of the midkine (MDK) gene.…”

Section: Introductionmentioning

confidence: 99%

Midkine release during hemodialysis is predictive of hypervolemia and associates with excess (cardiovascular) mortality in patients with end-stage renal disease: a prospective study

et al. 2022

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Background In end-stage renal disease, a high cardiovascular risk profile and endothelial damage prevails. The heparin-binding growth factor midkine stimulates neo-angiogenesis in ischemic diseases, coordinates neutrophil influx, and raises blood pressure through stimulated angiotensin synthesis. Methods We determined changes of midkine serum levels during hemodialysis sessions under the assumption that endothelial cell-derived midkine is released. Periprocedural differences (∆midkine) were calculated and correlated with cardiovacular biomarkers and fluid status (clinical assessment, V. cava collapse, comet tail phenomenon), cardiovascular morbidities, mortality rates. Blood was collected before and after dialysis from hemodialysis patients (n = 171; diabetes: n = 70; hypervolemia: n = 83; both: n = 32). Results Baseline midkine levels were ~ fourfold elevated compared to healthy controls (n = 100). Further, on average a tenfold rise was detected during dialysis, the extent of which was partially related to non-fractionated heparin application (r2 = 0.17). Inter-individual differences were highly reproducible. Hypervolemic patients responded with a less than average rise in midkine levels during dialysis (p < 0.02), this difference became more obvious with co-existing diabetes (p < 0.001 for long dialysis-free interval) and was confirmed in an independently enrolled dialysis cohort (n = 88). In Kaplan Meier survival curves, low delta midkine levels correlated with cardiovascular/overall mortality rates, similar to elevated uPAR levels, whereas other markers (NTproANP, galectin, tenascin-C) were less predictive. Following intervention with successful fluid removal in hypervolemic dialysis patients to optimize fluid homeostasis, midkine values increased (p < 0.002), which was not observed in patients that failed to decrease weight. Conclusion Thus, for dialysis patients inadequate periprocedural midkine upregulation is linked with hypervolemia and associates with cardiovascular events.

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Midkine rewires the melanoma microenvironment toward a tolerogenic and immune-resistant state

Cited by 84 publications

References 66 publications

Live imaging of neolymphangiogenesis identifies acute antimetastatic roles of dsRNA mimics

Live imaging of neolymphangiogenesis identifies acute antimetastatic roles of dsRNA mimics

Inactivation of EGLN3 hydroxylase facilitates Erk3 degradation via autophagy and impedes lung cancer growth

Midkine release during hemodialysis is predictive of hypervolemia and associates with excess (cardiovascular) mortality in patients with end-stage renal disease: a prospective study

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