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Tytuł:
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Preclinical safety and antitumor activity of the arginine-degrading therapeutic enzyme pegzilarginase, a PEGylated, cobalt-substituted recombinant human arginase 1.
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Autorzy:
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Agnello G; Aeglea BioTherapeutics, Inc., Austin, Texas.
Alters SE; Aeglea BioTherapeutics, Inc., Austin, Texas.
Rowlinson SW; Aeglea BioTherapeutics, Inc., Austin, Texas. Electronic address: .
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Źródło:
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Translational research : the journal of laboratory and clinical medicine [Transl Res] 2020 Mar; Vol. 217, pp. 11-22. Date of Electronic Publication: 2019 Dec 27.
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Typ publikacji:
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Journal Article; Research Support, Non-U.S. Gov't
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Język:
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English
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Imprint Name(s):
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Original Publication: New York, N.Y. : Elsevier, [2006]-
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MeSH Terms:
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Antineoplastic Agents/*pharmacology
Arginase/*pharmacology
Animals ; Arginase/analysis ; Arginase/toxicity ; Female ; Humans ; Macaca fascicularis ; Male ; Mice ; Mice, Inbred ICR ; Neoplasms, Experimental/drug therapy ; Neoplasms, Experimental/enzymology ; Recombinant Proteins/pharmacology ; Xenograft Model Antitumor Assays
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Substance Nomenclature:
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0 (Antineoplastic Agents)
0 (Recombinant Proteins)
EC 3.5.3.1 (ARG1 protein, human)
EC 3.5.3.1 (Arginase)
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Entry Date(s):
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Date Created: 20200119 Date Completed: 20200925 Latest Revision: 20210405
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Update Code:
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20240104
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DOI:
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10.1016/j.trsl.2019.12.005
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PMID:
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31954097
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Metabolic remodeling contributes to the development and progression of some cancers and exposes them to vulnerabilities, including specific nutrient dependencies that can be targeted therapeutically. Arginine is a semiessential amino acid, and several cancers are unable to endogenously synthesize sufficient levels of arginine for survival and proliferation, most commonly due to reduced expression of argininosuccinate synthase (ASS1). Such cancers are dependent on arginine and they can be targeted via enzyme-mediated depletion of systemic arginine. We report the preclinical safety, antitumor efficacy, and immune-potentiating effects of pegzilarginase, a highly potent human arginine-degrading enzyme. Toxicology studies showed that pegzilarginase-mediated arginine depletion is well tolerated at therapeutic levels that elicit an antitumor growth effect. To determine which tumor types are best suited for clinical development, we profiled clinical tumor samples for ASS1 expression, which correlated with pegzilarginase sensitivity in vivo in patient-derived xenograft (PDx) models. Among the histologies tested, malignant melanoma, small cell lung cancer and Merkel cell carcinoma had the highest prevalence of low ASS1 expression, the highest proportion of PDx models responding to pegzilarginase, and the strongest correlation between low or no ASS1 expression and sensitivity to pegzilarginase. In an immune-competent syngeneic mouse model, pegzilarginase slowed tumor growth and promoted the recruitment of CD8 + tumor infiltrating lymphocytes. This is consistent with the known autophagy-inducing effects of arginine depletion, and the link between autophagy and major histocompatibility complex antigen presentation to T cells. Our work supports the ongoing clinical investigations of pegzilarginase in solid tumors and clinical combination of pegzilarginase with immune checkpoint inhibitors.
(Copyright © 2020 Elsevier Inc. All rights reserved.)
