Small molecule inhibitors of ER α-glucosidases are active against multiple hemorrhagic fever viruses

Chang, Jinhong; Warren, Travis K.; Zhao, Xiongyan; Gill, Tina; Guo, Fang; Wang, Limin; Comunale, Mary Ann; Du, Yanming; Alonzi, Dominic S.; Yu, Wenquan; Ye, Hong; Liu, Fei; Guo, Ju‐Tao; Mehta, Anand; Cuconati, Andrea; Butters, Terry D.; Bavari, Sina; Xu, Xiaodong; Block, Timothy M.

doi:10.1016/j.antiviral.2013.03.023

Cited by 80 publications

(105 citation statements)

References 43 publications

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“…Iminosugars, glycomimetics originally isolated from plants, represent a promising class of ERQC inhibitors that are well tolerated in mammals (13). Altering glycoprotein processing via inhibition of the ER α-GluI and α-GluII by iminosugars has demonstrated in vitro and in vivo efficacy against multiple virus families (14, 15), including Herpes-, Hepadna-, Toga-, Rhabdo-, Orthomyxo-, Paramyxo-and Retroviridae, as well as those virus families that cause hemorrhagic fever (16,17), including Arena-, Flavi-and Filoviridae. The deoxynojirimycin iminosugar derivative N-9′-methoxynonyl 1-deoxynojirimycin (MON-DNJ) has antiviral activity in vivo, against both dengue virus (18) and influenza A (H1N1) (19) and influenza B (17), with the Significance Most pathogenic enveloped viruses crucially depend on the quality control (QC) machinery in the endoplasmic reticulum (ER) of the host cell.…”

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confidence: 99%

Structures of mammalian ER α-glucosidase II capture the binding modes of broad-spectrum iminosugar antivirals

Caputo

Alonzi

Marti

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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The biosynthesis of enveloped viruses depends heavily on the host cell endoplasmic reticulum (ER) glycoprotein quality control (QC) machinery. This dependency exceeds the dependency of host glycoproteins, offering a window for the targeting of ERQC for the development of broad-spectrum antivirals. We determined smallangle X-ray scattering (SAXS) and crystal structures of the main ERQC enzyme, ER α-glucosidase II (α-GluII; from mouse), alone and in complex with key ligands of its catalytic cycle and antiviral iminosugars, including two that are in clinical trials for the treatment of dengue fever. The SAXS data capture the enzyme's quaternary structure and suggest a conformational rearrangement is needed for the simultaneous binding of a monoglucosylated glycan to both subunits. The X-ray structures with key catalytic cycle intermediates highlight that an insertion between the +1 and +2 subsites contributes to the enzyme's activity and substrate specificity, and reveal that the presence of D-mannose at the +1 subsite renders the acid catalyst less efficient during the cleavage of the monoglucosylated substrate. The complexes with iminosugar antivirals suggest that inhibitors targeting a conserved ring of aromatic residues between the α-GluII +1 and +2 subsites would have increased potency and selectivity, thus providing a template for further rational drug design.broad-spectrum antiviral | ER α-glucosidase II | eukaryotic secretion | glycoprotein folding | iminosugar

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mentioning

confidence: 99%

Structures of mammalian ER α-glucosidase II capture the binding modes of broad-spectrum iminosugar antivirals

Caputo

Alonzi

Marti

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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“…ER α-glucosidases I and II play a critical role in glycosylation of viral proteins 102 . Inhibition of ER α-glucosidases has shown to affect viral particle assembly and/or secretion of HBV, HIV, HSV-1, influenza virus, parainfluenza virus, measles virus (MV), MARV, EBOV, HCV and other members of the Flaviviridae, such as bovine viral diarrhea virus (BVDB), DENV, WNV, and japanese encephalitis virus (JEV) 117 . Celgosivir has been proven effective against HCV and DENV infections in vitro and in vivo 118,119 .…”

Section: Targeting Common Host-factors Used For Viral Replicationmentioning

confidence: 99%

“…CST, its derivative celgosivir (6 O-butanoyl castanospermine) and DNJ have been described to inhibit the replication of multiple viruses both in vitro and in vivo [117][118][119][187][188][189][190][191][192][193][194][195][196][197] (Table 2). In mammalian cells both compounds block the function of ER α-glucosidases I and II.…”

Section: Bsas Derived From Plants: Castanospermine 1-deoxynojirimycimentioning

confidence: 99%

Antiviral drug discovery: broad-spectrum drugs from nature

et al. 2015

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, but cannot be converted to PDF. You must view these files (e.g. movies) online.Scheme 1_(structures 1-5)_named.cdx Scheme 2_(structures 6-8)_named.cdx Scheme 3_(structure 9)_named.cdx Scheme 4_(structure 10)_named.cdx Scheme 5_ (structures 11-12) The development of drugs with broad-spectrum antiviral activities is a long pursued goal in drug discovery. It has been shown that blocking co-opted host-factors abrogates the replication of many viruses, yet the development of such host-targeting drugs has been met with skepticism mainly due to toxicity issues and poor translation to in vivo models. With the advent of new and more powerful screening assays and prediction tools, the idea of a drug that can efficiently treat a wide range of viral infections by blocking specific host functions has rebloomed. Here we critically review the state-of-the-art in broad-spectrum antiviral drug discovery. We discuss putative targets and treatment strategies, taking particular focus on natural products as promising starting points for antiviral lead development.

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“…Endoplasmic reticulum (ER) glucosidase inhibitors The imino sugar 1-deoxynojirimycin is a glucose mimic, with a nitrogen atom replacing the oxygen, that inhibits the ER α-glucosidases I and II, which are essential in the maturation of viral envelope glycoproteins (64). Its derivatives IHVR11029, IHVR17028 and IHVR19029 were shown to protect mice against the mortality of Marburg and EBOV infections (65). Benzylpiperazine adamantane diamides EBOV entry into the host cells requires the cholesterol transporter Niemann-Pick C1 (66), and this process can be blocked by benzylpiperazine adamantane diamides (67).…”

Section: Ebov Inhibitors Interacting With Viral Entry (Fig 9)mentioning

confidence: 99%

Vesicular stomatitis virus (VSV) as a paradigm for predicting antiviral activity against Ebola virus (EBOV)

Clercq

2015

mpj

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There are at present no antivirals available which have been formally licensed for clinical use for the treatment of Ebola virus (EBOV) infections in humans. The most advanced to be approved for this purpose is favipiravir (T-705), a viral RNA polymerase inhibitor. Under consideration are BCX4430, also a viral RNA polymerase inhibitor, and 3-deazaneplanocin A and various other S-adenosylhomocysteine (SAH) hydrolase inhibitors. A number of compounds which have been approved for other purposes seem to interact with the cell entry of EBOV. Some compounds like pyrazofurin have been found to be exquisitely potent inhibitors of vesicular stomatitis virus (VSV). VSV belongs to the rhabdoviridae, a family closely related to the family of the filoviridae to which EBOV and Marburg virus belong. VSV, unlike EBOV and Marburg virus which require biosafety level 4, can be handled in conventional safety conditions.

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Small molecule inhibitors of ER α-glucosidases are active against multiple hemorrhagic fever viruses

Cited by 80 publications

References 43 publications

Structures of mammalian ER α-glucosidase II capture the binding modes of broad-spectrum iminosugar antivirals

Structures of mammalian ER α-glucosidase II capture the binding modes of broad-spectrum iminosugar antivirals

Antiviral drug discovery: broad-spectrum drugs from nature

Vesicular stomatitis virus (VSV) as a paradigm for predicting antiviral activity against Ebola virus (EBOV)

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