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3 research outputs found

SARS-CoV-2 infects the human kidney and drives fibrosis in kidney organoids

Author: Achdout H.
Aimon A.
Akiva A.
Alexandrov T.
Bar-David E.
Barr H.
Ben-Shmuel A.
Bennett J.
Beukenboom M.
Bindels E.M.J.
Boby M.L.
Boor P.
Borden B.
Bowman G.R.
Brun J.
Bulthuis M.
BVNBS S.
Calmiano M.
Carbery A.
Cattermole E.
Chernychenko E.
Choder J.D.
Clyde A.
Coffland J.E.
Cohen G.
Cole J.
Contini A.
Costa I.G.
Cox L.
Cvitkovic M.
Czogalla J.
Daviran D.
de Beer M.
De Jonghe S.
Dias A.
Djudjaj S.
Donckers K.
Dotson D.L.
Douangamath A.
Duberstein S.
Dudgeon T.
Dunnen W.D.
Dunnett L.
Eastman P.K.
Erez N.
Eyermann C.J.
Fairhead M.
Fate G.
Fearon D.
Federov O.
Ferla M.
Fermin L.A.S.
Fernandes R.S.
Ferrins L.
Floege J.
Foster H.
Foster R.
Gabizon R.
Garcia-Sastre A.
Gawriljuk V.O.
Gehrtz P.
Gileadi C.
Giroud C.
Glass W.G.
Glen R.
Godoy A.S.
Gorichko M.
Gorrie-Stone T.
Griffen E.J.
Grünberg K.
Hart S.H.
Heer J.
Heijnert J.
Henry M.
Hill M.
Hillebrands J.-L.
Hoogenboezem R.M.
Horrell S.
Huber T.B.
Hurley M.F.D.
Ijzermans T.
Israely T.
Itai glinert
Jajack A.
Jansen J.
Jnoff E.
Jochmans D.
John T.
Kantsadi A.L.
Kenny P.W.
Kiappes J.L.
Koekemoer L.
Kovar B.
Kramann R.
Krojer T.
Kuppe C.
Lee A.A.
Lefker B.A.
Levy H.
London N.
Lukacik P.
Macdonald H.B.
Maclean B.
Malla T.R.
Mastik M.
Matviiuk T.
McCorkindale W.
McGovern B.L.
Melamed S.
Michurin O.
Miesen P.
Mikolajek H.
Milne B.F.
Mooren F.
Morris A.
Morris G.M.
Morwitzer M.J.
Moustakas D.
Nagai J.S.
Nakamura A.M.
Neto J.B.
Neyts J.
Nguyen L.
Nlandu Q.
Noske G.D.
Oleinikovas V.
Oliva G.
Overheul G.J.
Overheul G.J.
Owen D.
Pai R.
Pan J.
Paran N.
Perry B.
Pingle M.
Pinjari J.
Politi B.
Powell A.
Psenak V.
Puelles V.G.
Puni R.
Rangel V.L.
Reddi R.N.
Reid S.P.
Reimer K.C.
Resnick E.
Ripka E.G.
Robinson M.C.
Robinson R.P.
Rodriguez-Guerra J.
Rosales R.
Roverts R.
Rufa D.
Schneider R.K.
Schofield C.
Schreuder M.F.
Shafeev M.
Shaikh A.
Shi J.
Shurrush K.
Sing S.
Sittner A.
Skyner R.
Smalley A.
Smeets B.
Smilova M.D.
Solmesky L.J.
Sommerdijk N.
Spencer J.
Steenbergen E.J.
Strain-Damarell C.
Swamy V.
Tamir H.
Tennant R.
Thompson A.
Thompson W.
Thompson W.
Timm M.-C.
Tomasia S.
Triana S.H.
Tumber A.
Vakonakis I.
van den Berge B.T.
van den Broek M.
van Eijk L.E.
van Geel L.
van Goor H.
van Rij R.P.
van Rij R.P.
Varghese F.S.
Varghese F.S.
Vaschetto M.
Vitner E.B.
Voelz V.
Volkamer A.
von Delft A.
von Delft F.
von Stillfried S.
Walsh M.
Ward W.
Weatherall C.
Weiss S.
White K.M.
Wild C.F.
Willemsen B.
Wittmann M.
Wright N.
Yahalom-Ronen Y.
Zaidmann D.
Zidane H.
Zitzmann N.
Publication venue: Elsevier
Publication date: 03/02/2022
Field of study

Kidney failure is frequently observed during and after COVID-19, but it remains elusive whether this is a direct effect of the virus. Here, we report that SARS-CoV-2 directly infects kidney cells and is associated with increased tubule-interstitial kidney fibrosis in patient autopsy samples. To study direct effects of the virus on the kidney independent of systemic effects of COVID-19, we infected human-induced pluripotent stem-cell-derived kidney organoids with SARS-CoV-2. Single-cell RNA sequencing indicated injury and dedifferentiation of infected cells with activation of profibrotic signaling pathways. Importantly, SARS-CoV-2 infection also led to increased collagen 1 protein expression in organoids. A SARS-CoV-2 protease inhibitor was able to ameliorate the infection of kidney cells by SARS-CoV-2. Our results suggest that SARS-CoV-2 can directly infect kidney cells and induce cell injury with subsequent fibrosis. These data could explain both acute kidney injury in COVID-19 patients and the development of chronic kidney disease in long COVID

White Rose Research Online

Transmittance and reflectance measurements at terahertz frequencies on a superconducting BaFe1.84Co0.16As2 ultrathin film: an analysis of the optical gaps in the Co-doped BaFe2As2 pnictide

Author: A. Charnukha
A. Dusza
A. Lucarelli
A. Nicholson
A. Perucchi
A. Perucchi
A. Perucchi
A. Yu
A.A. Schafgans
A.B. Kuzmenko
Andrea Perucchi
B. Gorshunov
Boby Joseph
Chang Beom Eom
Chang Liu
D. Daghero
D. Nakamura
D. Wu
D.M. Ginsberg
D.N. Basov
D.S. Isonov
E. van Heumen
E.G. Maksimov
E.G. Maksimov
Eric E. Hellstrom
F. Hardy
Fa Wang
H. Suhl
H.H. Wen
I.I. Mazin
J.J. Tu
J.P. Hirschfeld
Jeremy D. Weiss
Jianyi Jiang
Jiun-Haw Chu
K. Terashima
K.W. Kim
L. Baldassarre
L. Benfatto
L.H. Palmer
Leonetta Baldassarre
M. Misra
M. Nakajima
M. Ortolani
M. Ortolani
M. Tortello
M.L. Teague
N. Barisic
O.K. Andersen
P. Berberich
P. Dore
P. Dore
P. Dore
P. Marsik
P. Richard
P. Vilmercati
P.C. Canfield
Paolo Dore
Q. Han
R. Valdés Aguilar
R.E. Glover
R.P.S.M. Lobo
S. Lee
S. Lupi
S. Lupi
S. Raghu
S. Thirupathaiah
S.J. Moon
Sanghan Lee
Stefano Lupi
T. Fischer
T. Sudayama
W. Zimmermann
X. Xi
X.X. Xi
Y. Kamihara
Y. Zhang
Z.-A. Ren
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Open science discovery of potent noncovalent SARS-CoV-2 main protease inhibitors

Author: Achdout H.
Aimon A.
Alonzi D.S.
Arbon R.
Aschenbrenner J.C.
Balcomb B.H.
Bar-David E.
Barr H.
Ben-Shmuel A.
Bennett J.
Bilenko V.A.
Boby M.L.
Borden B.
Boulet P.
Bowman G.R.
Brewitz L.
Brun J.
BVNBS S.
Calmiano M.
Carbery A.
Carney D.W.
Cattermole E.
Chang E.
Chernyshenko E.
Chodera J.D.
Clyde A.
Coffland J.E.
Cohen G.
Cole J.C.
Contini A.
Cox L.
Croll T.I.
Cvitkovic M.
De Jonghe S.
Dias A.
Donckers K.
Dotson D.L.
Douangamath A.
Duberstein S.
Dudgeon T.
Dunnett L.E.
Eastman P.
Erez N.
Eyermann C.J.
Fairhead M.
Fate G.
Fearon D.
Fedorov O.
Ferla M.
Fernandes R.S.
Ferrins L.
Filep M.
Foster H.
Foster R.
Fraisse L.
Gabizon R.
García-Sastre A.
Gawriljuk V.O.
Gehrtz P.
Gileadi C.
Giroud C.
Glass W.G.
Glen R.C.
Glinert I.
Godoy A.S.
Gorichko M.
Gorrie-Stone T.
Griffen E.J.
Haneef A.
Hassell Hart S.
Heer J.
Henry M.
Hill M.
Horrell S.
Huang Q.Y.J.
Huliak V.D.
Hurley M.F.D.
Israely T.
Jajack A.
Jansen J.
Jnoff E.
Jochmans D.
John T.
Kaminow B.
Kang L.
Kantsadi A.L.
Kenny P.W.
Kiappes J.L.
Kinakh S.O.
Koekemoer L.
Kovar B.
Krojer T.
La V.N.T.
Laghnimi-Hahn S.
Lee A.A.
Lefker B.A.
Levy H.
Lithgo R.M.
Logvinenko I.G.
London N.
Lukacik P.
Macdonald H.B.
MacLean E.M.
Makower L.L.
Malla T.R.
Marples P.G.
Matviiuk T.
McCorkindale W.
McGovern B.L.
Melamed S.
Melnykov K.P.
Michurin O.
Miesen P.
Mikolajek H.
Milne B.F.
Minh D.
Morris A.
Morris G.M.
Morwitzer M.J.
Moustakas D.
Mowbray C.E.
Nakamura A.M.
Neto J.B.
Neyts J.
Nguyen L.
Noske G.D.
Oleinikovas V.
Oliva G.
Overheul G.J.
Owen C.D.
Pai R.
Pan J.
Paran N.
Payne A.M.
Perry B.
Pingle M.
Pinjari J.
Politi B.
Powell A.
Pulido I.
Puni R.
Pšenák V.
Rangel V.L.
Reddi R.N.
Rees P.
Reid L.
Reid S.P.
Resnick E.
Ripka E.G.
Robinson M.C.
Robinson R.P.
Rodriguez-Guerra J.
Rosales R.
Rufa D.A.
Saar K.
Saikatendu K.S.
Salah E.
Schaller D.
Scheen J.
Schiffer C.A.
Schofield C.J.
Shafeev M.
Shaikh A.
Shaqra A.M.
Shi J.
Shurrush K.
Singh S.
Sittner A.
Sjö P.
Skyner R.
Smalley A.
Smeets B.
Smilova M.D.
Solmesky L.J.
Spencer J.
Strain-Damerell C.
Swamy V.
Tamir H.
Taylor J.C.
Tennant R.E.
Thompson A.
Thompson W.
Tomlinson C.W.E.
Tomásio S.
Tsurupa I.S.
Tumber A.
Vakonakis I.
van Rij R.P.
Vangeel L.
Varghese F.S.
Vaschetto M.
Vitner E.B.
Voelz V.
Volkamer A.
von Delft A.
von Delft F.
Walsh M.A.
Ward W.
Weatherall C.
Weiss S.
White K.M.
Wild C.F.
Witt K.D.
Wittmann M.
Wright N.
Yahalom-Ronen Y.
Yilmaz N.K.
Zaidmann D.
Zhang I.
Zidane H.
Zitzmann N.
Zvornicanin S.N.
Publication venue: American Association for the Advancement of Science (AAAS)
Publication date: 10/11/2023
Field of study

We report the results of the COVID Moonshot, a fully open-science, crowdsourced, and structure-enabled drug discovery campaign targeting the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) main protease. We discovered a noncovalent, nonpeptidic inhibitor scaffold with lead-like properties that is differentiated from current main protease inhibitors. Our approach leveraged crowdsourcing, machine learning, exascale molecular simulations, and high-throughput structural biology and chemistry. We generated a detailed map of the structural plasticity of the SARS-CoV-2 main protease, extensive structure-activity relationships for multiple chemotypes, and a wealth of biochemical activity data. All compound designs (>18,000 designs), crystallographic data (>490 ligand-bound x-ray structures), assay data (>10,000 measurements), and synthesized molecules (>2400 compounds) for this campaign were shared rapidly and openly, creating a rich, open, and intellectual property–free knowledge base for future anticoronavirus drug discovery

White Rose Research Online