Immune checkpoint inhibition combined with targeted therapy using a novel virus-like drug conjugate induces complete responses in a murine model of local and distant tumors

Veld, Ruben V. Huis in ‘t; Ma, Sen; Kines, Rhonda C.; Savinainen, Anneli; Rich, Cadmus; Ossendorp, Ferry; Jager, Martine J.

doi:10.1007/s00262-023-03425-3

Cited by 13 publications

(8 citation statements)

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“…The International Classification of Diseases (ICD) and favorable microenvironment triggered by Bel-sar treatment are indicators for combination with immune check point inhibitors to induce the local and distant tumor cure. 16 , 17 , 63 Further preclinical and clinical studies to investigate the combination Bel-sar treatment and immune checkpoint inhibitors should be conducted. Our results indicate that despite the light-absorbing function of pigments, which was proposed to be detrimental for laser therapy, we could show that Bel-sar treatment can enhance antitumor immune effects even in pigmented malignancies.…”

Section: Discussionmentioning

confidence: 99%

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Tumor Pigmentation Does Not Affect Light-Activated Belzupacap Sarotalocan Treatment but Influences Macrophage Polarization in a Murine Melanoma Model

Ma,

Huis in't Veld,

Hao

et al. 2024

Invest. Ophthalmol. Vis. Sci.

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Purpose Pigmentation in uveal melanoma is associated with increased malignancy and is known as a barrier for photodynamic therapy. We investigated the role of pigmentation in tumor behavior and the response to light-activated Belzupacap sarotalocan (Bel-sar) treatment in a pigmented (wild type) and nonpigmented (tyrosinase knock-out [TYR knock-out]) cell line in vitro and in a murine model. Methods The B16F10 (TYR knock-out) was developed using CRISPR/Cas9. After the treatment with light-activated Bel-sar, cytotoxicity and exposure of damage-associated molecular patterns (DAMPs) were measured by flow cytometry. Treated tumor cells were co-cultured with bone marrow-derived macrophages (BMDMs) and dendritic cells (DCs) to assess phagocytosis and activation. Both cell lines were injected subcutaneously in syngeneic C57BL/6 mice. Results Knock-out of the tyrosinase gene in B16F10 led to loss of pigmentation and immature melanosomes. Pigmented tumors contained more M1 and fewer M2 macrophages compared with amelanotic tumors. Bel-sar treatment induced near complete cell death, accompanied with enhanced exposure of DAMPs in both cell lines, resulting in enhanced phagocytosis of BMDMs and maturation of DCs. Bel-sar treatment induced a shift to M1 macrophages and delayed tumor growth in both in vivo tumor models. Following treatment, especially the pigmented tumors and their draining lymph nodes contained IFN-gamma positive CD8+T cells. Conclusions Pigmentation influenced the type of infiltrating macrophages in the tumor, with more M1 macrophages in pigmented tumors. Belzupacap sarotalocan treatment induced immunogenic cell death and tumor growth delay in pigmented as well as in nonpigmented models and stimulated M1 macrophage influx in both models.

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Section: Discussionmentioning

confidence: 99%

“…We recently published a paper stating that combining either PDT or light-activated Belzupacap sarotalocan (Bel-sar) with an immune checkpoint inhibitor induces a better antitumor response in mice than either treatment alone. 16 , 17 …”

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confidence: 99%

Tumor Pigmentation Does Not Affect Light-Activated Belzupacap Sarotalocan Treatment but Influences Macrophage Polarization in a Murine Melanoma Model

Ma,

Huis in't Veld,

Hao

et al. 2024

Invest. Ophthalmol. Vis. Sci.

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“…Kim et al suggested that the combination of the rho-kinase (ROCK) inhibitor ripasudil, PD0L1 inhibitor, and local photodynamic therapy (PDT) could reduce the primary tumor burden and prevent metastasis in an orthotopic intraocular melanoma model [ 56 ]. A new virus-like drug conjugate (AU-011) and the inhibitor of the receptor for the hepatocyte growth factor (HGF) are also worth studying in systemic treatment combined with ICIs [ 57 , 58 ].…”

Section: Current Status Of Clinical Studies Regarding Icis In Patient...mentioning

confidence: 99%

“…With a similar conclusion, Kashyap et al also found a potential association between higher LAG3 expression and shorter metastasis-free survival [ 74 ]. An in vivo experiment by Huis In 't Veld et al showed a CR rate of 75% in a murine model with distant MC38 tumors after treatment with AU-011 and a LAG3 inhibitor [ 57 ]. Thus, by observing valuable results from in vitro and in vivo experiments, the clinical effect of antibodies against LAG3 in UM, especially in the process of tumor metastasis, deserves to be investigated and validated.…”

Section: Current Status Of Clinical Studies Regarding Icis In Patient...mentioning

confidence: 99%

The Future of Checkpoint Inhibitors in Uveal Melanoma: A Narrative Review

Wang,

Li,

Yin

2024

Ophthalmol Ther

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Introduction Immune checkpoint inhibitors have made tremendous progress over the last decade in the treatment of cutaneous melanoma, but their application in uveal melanoma treatment is less successful, owing in part to the immunological privilege of the eye and the liver, the most frequent site of metastasis. Nevertheless, the therapeutic outcomes reported currently are less pessimistic. Methods In this review, we provide an overview of recent studies of immune checkpoint inhibitors in uveal melanoma and its metastasis and classify studies in this field into three groups: monotherapy of immune checkpoint inhibitors, dual-agent immune checkpoint inhibitors, and immune checkpoint inhibitors combined with other systemic or regional therapies. Results Briefly, monotherapy with immune checkpoint inhibitors performed poorly. Dual-agent immune checkpoint inhibitors had slightly better outcomes than traditional treatments, especially in specific patient populations. As for the combination therapy, the combination with other systemic therapies did not show superiority over dual-agent immune checkpoint inhibitors, but combination with hepatic regional therapies was quite promising. Moreover, research on emerging checkpoints is currently limited to the stage of mechanistic studies. Conclusion We propose that immune checkpoint inhibitors remain alternative treatments for patients with uveal melanoma, but factors such as cost-effectiveness should also be taken into account. The combination therapy with immune checkpoint inhibitors deserves to be further explored.

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“… 9 , 30 We recently showed that treatment with AU-011 and ICIs induced an abscopal effect in a murine model using MC38 cells. 28 Prior in vitro tests showed that AU-011 worked well on UM cell lines.…”

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confidence: 99%

In Vitro Testing of the Virus-Like Drug Conjugate Belzupacap Sarotalocan (AU-011) on Uveal Melanoma Suggests BAP1-Related Immunostimulatory Capacity

Ma,

Huis In't Veld,

Houy

et al. 2023

Invest. Ophthalmol. Vis. Sci.

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Purpose The virus-like drug conjugate belzupacap sarotalocan (AU-011), currently under clinical investigation for first-line treatment of primary uveal melanoma (UM), shows enhanced tumor specificity by targeting heparan sulfate proteoglycans (HSPG). Such a treatment may potentially lead to systemic immune responses. We studied the potential of AU-011 treatment to induce immunogenic cell death as the first step to induce systemic immunity. Methods We determined binding and uptake of AU-011 in ten primary and metastatic UM cell lines. The subcellular location of AU-011 was assessed by fluorescence microscopy. Following light activation (wavelength 690 nm) of AU-011, the half-maximal effective concentration (EC 50 ) of AU-011 treatment and exposure of damage-associated molecular patterns (DAMPs) were assessed using flow cytometry. DAMPs were measured by RNAseq. Results Fluorescence microscopy revealed most of the AU-011 was present in the cytoplasm. AU-011 binding and uptake by UM cells increased over time, with a lower uptake in BAP1-negative than in BAP1-positive cell lines. AU-011 activation induced cell death across all UM cell lines with EC 50 values at picomolar concentrations. The AU-011 concentration and total light dose (J/cm 2 ) were the most important parameters for the observed cytotoxicity. Finally, light-activated AU-011 induced exposure of DAMPs calreticulin (CRT) and HSP90. CRT exposure by light-activated AU-011 as well as CRT RNA exposure were lower in BAP1-negative compared to BAP1-positive UM cell lines. Conclusions AU-011 treatment at low picomolar range induces immunogenic cell death in all 10 UM cell lines. The in vitro cytotoxicity was accompanied by exposure of DAMPs (HSP90 and CRT), suggesting AU-011 may contribute to the development of systemic immunity and be a suitable candidate for combination with immunotherapy in vivo. AU-011 treatment was more effective against BAP1-positive cell lines, with a lower EC 50 and higher CRT exposure.

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Immune checkpoint inhibition combined with targeted therapy using a novel virus-like drug conjugate induces complete responses in a murine model of local and distant tumors

Cited by 13 publications

References 38 publications

Tumor Pigmentation Does Not Affect Light-Activated Belzupacap Sarotalocan Treatment but Influences Macrophage Polarization in a Murine Melanoma Model

Tumor Pigmentation Does Not Affect Light-Activated Belzupacap Sarotalocan Treatment but Influences Macrophage Polarization in a Murine Melanoma Model

The Future of Checkpoint Inhibitors in Uveal Melanoma: A Narrative Review

In Vitro Testing of the Virus-Like Drug Conjugate Belzupacap Sarotalocan (AU-011) on Uveal Melanoma Suggests BAP1-Related Immunostimulatory Capacity

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