First-in-Human Phase I Study of PRS-050 (Angiocal), an Anticalin Targeting and Antagonizing VEGF-A, in Patients with Advanced Solid Tumors

Mross, Klaus; Richly, Heike; Fischer, Richard; Scharr, Dirk; Büchert, Martin; Stern, Angelika C.; Gille, Hendrik; Audoly, Laurent; Scheulen, M. E.

doi:10.1371/journal.pone.0083232

Cited by 46 publications

(32 citation statements)

References 54 publications

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“…Tear lipocalin is nominally produced in the lung so exogenous protein would not induce antibody formation. Lack of immunogenicity is a feature of one newly engineered anticalin, which is based on the calyx structure and promiscuous ligand binding of tear lipocalin [66]. In our case release of the drug at the target could be enhanced by a number of local conditions.…”

Section: Discussionmentioning

confidence: 96%

Antibacterial activity of rifamycins for M. smegmatis with comparison of oxidation and binding to tear lipocalin

Staudinger

Redl

Glasgow

2014

Biochimica et Biophysica Acta (BBA) - Proteins and Proteomics

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A mutant of Mycobacterium smegmatis is a potential class I model substitute for Mycobacterium tuberculosis. Because not all of the rifamycins have been tested in this organism, we determined bactericidal profiles for the 6 major rifamycin derivatives. The profiles closely mirrored that established for Mycobacterium tuberculosis. Rifalazil was confirmed to be the most potent rifamycin. Because the tuberculous granuloma presents a harshly oxidizing environment we explored the effects of oxidation on rifamycins. Mass spectrometry confirmed that three of the six major rifamycins showed autoxidation in the presence of trace metals. Oxidation could be monitored by distinctive changes including isosbestic points in the ultraviolet-visible spectrum. Oxidation of rifamycins abrogated antimycobacterial activity in Mycobacterium smegmatis. Protection from autoxidation was conferred by binding susceptible rifamycins to tear lipocalin, a promiscuous lipophilic protein. Rifalazil was not susceptible to autoxidation but was insoluble in aqueous. Solubility was enhanced when complexed to tear lipocalin and was accompanied by a spectral red shift. The positive solvatochromism was consistent with robust molecular interaction and binding. Other rifamycins also formed a complex with lipocalin, albeit to a lesser extent. Protection from oxidation and enhancement of solubility with protein binding may have implications for delivery of select rifamycin derivatives.

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Section: Discussionmentioning

confidence: 96%

Antibacterial activity of rifamycins for M. smegmatis with comparison of oxidation and binding to tear lipocalin

Staudinger

Redl

Glasgow

2014

Biochimica et Biophysica Acta (BBA) - Proteins and Proteomics

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“…Mechanisms of iron acquisition and retention are enhanced in cancer cells [9], and the expression of genes that regulate iron metabolism are predictive of cancer patient outcome [22]. As a consequence, iron chelation is under active investigation as a potential anti-tumor strategy [23,24].…”

Section: Discussionmentioning

confidence: 99%

“…We and others have observed that the synthesis of hepcidin by tumors acts in an autocrine fashion to decrease ferroportin and thus restrict iron efflux out of tumor cells, promoting tumoral iron retention [7,8]. Since iron promotes tumor cell proliferation and metastasis [9], blocking hepcidin synthesis represents a potential strategy for limiting tumor growth, and might represent an additional use for commercially developed hepcidin antagonists.…”

Section: Introductionmentioning

confidence: 99%

Effects of Anti-repulsive Guidance Molecule C (RGMc/Hemojuvelin) Antibody on Hepcidin and Iron in Mouse Liver and Tumor Xenografts

Lemler

Bk³

et al. 2016

Clin Exp Pharmacol

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Objective Hepcidin is a peptide hormone produced by the liver that regulates systemic iron homeostasis. Hepcidin is also synthesized by tumors, where it contributes to tumor growth by increasing the tumoral retention of iron. Targeted reduction of hepcidin may therefore be useful in reducing tumor growth. H5F9-AM8 is an antibody in preclinical development for the anemia of chronic disease that reduces hepcidin synthesis by binding to RGMc, a co-receptor involved in the transcriptional induction of hepcidin by BMP6. We explored the ability of H5F9-AM8 to act as an anti-tumor agent. Methods Effects of anti-hemojuvelin antibody on hepcidin synthesis were assessed by qRTPCR in tissue culture and in tumor xenografts and livers of mice treated with H5F9-AM8 or saline. Tumor growth was assessed using caliper measurements. Serum iron was measured colorimetrically and tissue iron was measured using western blotting and inductively coupled mass spectrometry. Results In tissue culture, the anti-hemojuvelin antibody H5F9-AM8 significantly reduced BMP6-stimulated hepcidin synthesis in HepG2 and other cancer cells. In mice, H5F9-AM8 reduced hepcidin in the liver and increased serum iron, total liver iron, and liver ferritin. Although hepcidin in tumors was also significantly decreased, H5F9-AM8 did not reduce tumor iron content, ferritin, or tumor growth. Conclusion Anti-hemojuvelin antibody successfully reduces hepcidin in both tumors and livers but has different effects in these target organs: it reduces iron content and ferritin in the liver, but does not reduce iron content or ferritin in tumors, and does not inhibit tumor growth. These results suggest that despite their ability to induce hepcidin in tumors, the anti-tumor efficacy of systemic, non-targeted hepcidin antagonists may be limited by their ability to simultaneously elevate plasma iron. Tumor-specific hepcidin inhibitors may be required to overcome the limitations of drugs that target the synthesis of both systemic and tumor hepcidin.

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“…[122] Another Anticalin developed by Pieris Pharmaceuticals, Inc. was well tolerated in a phase 1 trial. [123] Results are pending from a phase 1 clinical trial of PRS-080 which concluded this year. [124] Pending favorable results, Pieris Pharmaceuticals, Inc. intends to initiate phase 2 trials in patients with chronic kidney disease suffering from functional iron deficiency anemia.…”

Section: Hepcidin Antagonistsmentioning

confidence: 99%

Modulation of hepcidin to treat iron deregulation: potential clinical applications

Blanchette

Manz

Torti

et al. 2015

Expert Review of Hematology

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The secreted peptide hormone hepcidin regulates systemic and local iron homeostasis through degradation of the iron exporter ferroportin. Dysregulation of hepcidin leads to altered iron homeostasis and development of pathological disorders including hemochromatosis, and iron loading and iron restrictive anemias. Therapeutic modulation of hepcidin is a promising method to ameliorate these conditions. Several approaches have been taken to enhance or reduce the effects of hepcidin in vitro and in vivo. Based on these approaches, hepcidin modulating drugs have been developed and are undergoing clinical evaluation. In this article we review the rationale for development of these drugs, the data concerning their safety and efficacy, their therapeutic uses, and potential future prospects.

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First-in-Human Phase I Study of PRS-050 (Angiocal), an Anticalin Targeting and Antagonizing VEGF-A, in Patients with Advanced Solid Tumors

Cited by 46 publications

References 54 publications

Antibacterial activity of rifamycins for M. smegmatis with comparison of oxidation and binding to tear lipocalin

Antibacterial activity of rifamycins for M. smegmatis with comparison of oxidation and binding to tear lipocalin

Effects of Anti-repulsive Guidance Molecule C (RGMc/Hemojuvelin) Antibody on Hepcidin and Iron in Mouse Liver and Tumor Xenografts

Modulation of hepcidin to treat iron deregulation: potential clinical applications

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