Czech National Centre of the European Research Infrastructure Consortium INSTRUCT ERIC

19 Jan

Job position - Expert in scientific programming and data management

18 Jan

Emerging Topics in Biomolecular Magnetic Resonance - Wei Qiang (Binghamton University) and Rasmus Linser (Technical University Dortmund)

15 Jan

The 2021 ISMAR conference will be held during August 22-27

as a joint conference consisting of 22nd International Society of Magnetic Resonance Conference,  9th Asia-Pacific NMR Symposium, 60th Annual Meeting of the Nuclear Magnetic Resonance Society of Japan
and 60th Annual Meeting of the Society of Electron Spin Science and Technology. The conference will be held as a hybrid format of on-line and virtual events with options to participate in Osaka, Japan. The on-line
format will allow participants from all the time zones to interact actively. 

13 Jan

Papain-like protease regulates SARS-CoV-2 viral spread and innate immunity (Nature)

The papain-like protease PLpro is an essential coronavirus enzyme that is required for processing viral polyproteins to generate a functional replicase complex and enable viral spread. PLpro is also implicated in cleaving proteinaceous post-translational modifications on host proteins as an evasion mechanism against host antiviral immune responses. Here I. Dikic et. al.  perform biochemical, structural and functional characterization of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) PLpro (SCoV2-PLpro) and outline differences with SARS-CoV PLpro (SCoV-PLpro) in regulation of host interferon and NF-κB pathways. SCoV2-PLpro and SCoV-PLpro share 83% sequence identity but exhibit different host substrate preferences; SCoV2-PLpro preferentially cleaves the ubiquitin-like interferon-stimulated gene 15 protein (ISG15), whereas SCoV-PLpro predominantly targets ubiquitin chains. The crystal structure of SCoV2-PLpro in complex with ISG15 reveals distinctive interactions with the amino-terminal ubiquitin-like domain of ISG15, highlighting the high affinity and specificity of these interactions. Furthermore, upon infection, SCoV2-PLpro contributes to the cleavage of ISG15 from interferon responsive factor 3 (IRF3) and attenuates type I interferon responses. Notably, inhibition of SCoV2-PLpro with GRL-0617 impairs the virus-induced cytopathogenic effect, maintains the antiviral interferon pathway and reduces viral replication in infected cells. These results highlight a potential dual therapeutic strategy in which targeting of SCoV2-PLpro can suppress SARS-CoV-2 infection and promote antiviral immunity.

13 Jan

An ultrapotent synthetic nanobody neutralizes SARS-CoV-2 by stabilizing inactive Spike (Science)

The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) virus enters host cells via an interaction between its Spike protein and the host cell receptor angiotensin-converting enzyme 2 (ACE2). By screening a yeast surface-displayed library of synthetic nanobody sequences, QCRG Structural Biology Consortiumdeveloped nanobodies that disrupt the interaction between Spike and ACE2. Cryo–electron microscopy (cryo-EM) revealed that one nanobody, Nb6, binds Spike in a fully inactive conformation with its receptor binding domains locked into their inaccessible down state, incapable of binding ACE2. Affinity maturation and structure-guided design of multivalency yielded a trivalent nanobody, mNb6-tri, with femtomolar affinity for Spike and picomolar neutralization of SARS-CoV-2 infection. mNb6-tri retains function after aerosolization, lyophilization, and heat treatment, which enables aerosol-mediated delivery of this potent neutralizer directly to the airway epithelia.