alpha

Alphacool Apex Pro Skeleton Carbon Case Featured Build and more @ NT Compatible

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U.N. force: Israel building on so-called Alpha Line with Syria saw 'severe violations' of cease-fire

United Nations peacekeepers warned Tuesday that the Israeli military has committed "severe violations" of a cease-fire deal with Syria as its military continues a major construction project along the so-called Alpha Line that separates the Israeli-occupied Golan Heights from Syria.




alpha

DINA Technical Workshop - Alpha version of mobilization system

Target group: programmers, developers and system engineers. The workshop is open to anybody who might be interested to learn more about the DINA-system.

Preliminary agenda:

  • Presentations from all DINA-partners
  • APIs, service oriented architecture and road map for distributed development, guidelines and principles on how to build a module and join the DINA-system
  • Case studies
  • Delivery options: creating installations from hosted environment, virtual machines down to code.

A detailed program will be available by the end of August 2014.

There will be a SETF-meeting for DINA consortium members on the 15th of September.

Welcome to register for the workshop here:

DINA - Technical Workshop 16-18 September, Stockholm

The workshop is an activity within WP 1 Task 1.4





alpha

DINA Technical Workshop - Alpha version of mobilization system

Target group: programmers, developers and system engineers. The workshop is also open to anybody who might be interested to learn more about the DINA-system.

Preliminary agenda:

  • Presentations from all DINA-partners
  • APIs, service oriented architecture and road map for distributed development guidelines and principles on how to build a module and join the DINA-system
  • Case studies
  • Delivery options: creating installations from hosted environment, virtual machines down to code.

Workshop Program.

There will be a SETF-meeting for DINA consortium members on the 15th of September.

Welcome to register for the workshop here:

DINA - Technical Workshop 16-18 September, Stockholm

The workshop is an activity within WP 1 Task 1.4





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EUBON Workshop Milestone 144: Alpha version of data mobilization systems online

Workshop on beta versions of data mobilization systems at the Swedish Museum of Natural History, Stockholm.

Registration link: http://goo.gl/forms/pCvjglXpcN

 

 

 





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Accounting for biotic interaction though alpha-diversity constraints in stacked species distribution models




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Global study from Checkout.com reveals Generation Alpha’s rising influence in Digital Economy

A global study by Checkout.com, the global digital payments company, highlights the consumer buying behaviour which is powering today’s digital economy. The research, conducted across the UK, US, UAE and China, reveals a number of trends, including the growing spending power of Generation Alpha.




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Gov't Designates '2024 Hangeul Week' to Celebrate Creation of Korean Alphabet

[Culture] :
The government has designated the seven days from Friday to next Thursday as the "2024 Hangeul Week," on the occasion of the 578th Hangeul Day on October 9 to mark the creation of the Korean alphabet. According to the culture ministry on Monday, a number of cultural events that can help participants better ...

[more...]




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PM Han in Hangeul Day Speech: Nation Has Duty to Further Develop Korean Alphabet

[Culture] :
Prime Minister Han Duck-soo said the nation has a duty to further develop the Korean alphabet, hangeul, which has gained worldwide recognition as a unique writing system. At a government ceremony marking the 578th Hangeul Day on Wednesday, Han raised concerns about “indifference to the Korean language” ...

[more...]




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AlphaFold-assisted structure determination of a bacterial protein of unknown function using X-ray and electron crystallography

Macromolecular crystallography generally requires the recovery of missing phase information from diffraction data to reconstruct an electron-density map of the crystallized molecule. Most recent structures have been solved using molecular replacement as a phasing method, requiring an a priori structure that is closely related to the target protein to serve as a search model; when no such search model exists, molecular replacement is not possible. New advances in computational machine-learning methods, however, have resulted in major advances in protein structure predictions from sequence information. Methods that generate predicted structural models of sufficient accuracy provide a powerful approach to molecular replacement. Taking advantage of these advances, AlphaFold predictions were applied to enable structure determination of a bacterial protein of unknown function (UniProtKB Q63NT7, NCBI locus BPSS0212) based on diffraction data that had evaded phasing attempts using MIR and anomalous scattering methods. Using both X-ray and micro-electron (microED) diffraction data, it was possible to solve the structure of the main fragment of the protein using a predicted model of that domain as a starting point. The use of predicted structural models importantly expands the promise of electron diffraction, where structure determination relies critically on molecular replacement.




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The success rate of processed predicted models in molecular replacement: implications for experimental phasing in the AlphaFold era

The availability of highly accurate protein structure predictions from AlphaFold2 (AF2) and similar tools has hugely expanded the applicability of molecular replacement (MR) for crystal structure solution. Many structures can be solved routinely using raw models, structures processed to remove unreliable parts or models split into distinct structural units. There is therefore an open question around how many and which cases still require experimental phasing methods such as single-wavelength anomalous diffraction (SAD). Here, this question is addressed using a large set of PDB depositions that were solved by SAD. A large majority (87%) could be solved using unedited or minimally edited AF2 predictions. A further 18 (4%) yield straightforwardly to MR after splitting of the AF2 prediction using Slice'N'Dice, although different splitting methods succeeded on slightly different sets of cases. It is also found that further unique targets can be solved by alternative modelling approaches such as ESMFold (four cases), alternative MR approaches such as ARCIMBOLDO and AMPLE (two cases each), and multimeric model building with AlphaFold-Multimer or UniFold (three cases). Ultimately, only 12 cases, or 3% of the SAD-phased set, did not yield to any form of MR tested here, offering valuable hints as to the number and the characteristics of cases where experimental phasing remains essential for macromolecular structure solution.




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2024 Bakery of the Year: Alpha Baking Co.

The brand’s unique products have made it a Chicago staple.




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alphaMountain Adds New URL Classification Categories to AI-Powered Domain and IP Threat Intelligence Data

New categories empower cybersecurity technology providers and researchers with high-fidelity website classification for threat investigations and real-time policy enforcement




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GRE Alpha's DC Voltage Drop Calculator Celebrates Six Years of Service

In its Sixth Year Over 100,000 Users Have Benefited from This Essential Voltage Drop Calculator




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Artsyl Technologies Unveils docAlpha 7.0, the Latest Release of Intelligent Process Automation Platform

Revolutionizing Document-Based Business Process Automation for Enhanced Efficiency and Accuracy.




alpha

GRE Alpha's Voltage Drop Calculator Celebrates Sixth Anniversary

GRE Voltage Drop Calculator Celebrates Third Year Of Maximizing Energy Efficiency for LED Lighting Systems




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alphaMountain Launches threatYeti, a Cybersecurity Research Platform for Domains and IPs

One-Click Threat Intelligence and Real-Time Verdicts Empower Security Researchers and Analysts of All Skill Levels




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GRE Alpha Engages Global Lighting and Controls to Amplify the Promotion of LED Power Supplies and Lighting Controls

GRE Alpha North America and Global Lighting and Controls (GL&C) have announced their partnership.




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GRE Alpha's Voltage Drop Calculator Hits Milestone: Over 10K Users in 2024

The essential tool for efficient power management celebrates a significant user milestone, reflecting its growing impact in the industry




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GRE Alpha Partners With Japan Display Inc. On LumiFree Lighting Technology

LumiFree allows users to control the light distribution characteristics of lighting at any given time




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3NUM, Inventor of the Web3 Mobile Number, Launches New Secure Second Phone App Alpha - 'Speak.3Z'

Austin-based 3NUM, a trailblazer in secure web3 native communication, invites users to join the waitlist for its innovative app called Speak.3Z combining onchain and traditional phone capabilities.




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K-12 Game-based Learning Market is to grow by USD 16.50 billion from 2022 to 2027, the market is fragmented due to the presence of companies like Alphabet Inc., Banzai Labs Inc. & BrainQuake

Exploring the Dynamic Landscape of the K-12 Game-based Learning Market: A Comprehensive Analysis of Growth Trends, Key Players, and Market Fragmentation from 2022 to 2027




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GRE Alpha's Dimming Modules Power a Luxurious Atmosphere at the Janu Hotel in Tokyo, Japan

Janu Hotel wanted to create an unforgettable ambiance and experience for guests in the lobby




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AlphaOmega Style Now Accepting Appointments at the Salon and Spa Galleria Six Flags in Arlington, Texas

Owner Shuntay Smith provides weaves, silk press, crochet braid styles, protective styles, sew-ins, micro-link bead extensions, natural hair treatments, and more.




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Alphabet CEO Sundar Pichai on Leadership, AI, and Big Tech

The use of artificial intelligence and specifically generative AI is growing rapidly, and tech giants like Google have an important role to play in how that technology gets adopted and developed. Sundar Pichai is the CEO of Google as well as its parent company Alphabet, which he's led as an AI-first company for several years. He speaks with HBR editor in chief Adi Ignatius about shaping Google's AI strategy, putting safeguards in place, and how work and leadership will change as AI advances.




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Divi 5 Public Alpha Progress Update (200+ Changes)

Last month, we released the Divi 5 Public Alpha, and we’ve been 100% focused on fixing the bugs you’ve been reporting. We released two new versions (Public Alpha Version 1 and Public Alpha Version Two), including over 200 bug fixes and improvements. Download The Divi 5 Alpha Next Stop, Stability We have our eyes set […]

The post Divi 5 Public Alpha Progress Update (200+ Changes) appeared first on Elegant Themes Blog.




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Divi 5 Update: Public Alpha Version 3

The Divi 5 Public Alpha is available for testing. As we progress towards the final release, we’ll update Divi 5 every two weeks, appearing as a standard update in your WordPress dashboard. If you use Divi 5, you’ll notice an update notification for Public Alpha Version 3 today. Thanks to everyone who has reported bugs so […]

The post Divi 5 Update: Public Alpha Version 3 appeared first on Elegant Themes Blog.





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ASUS ROG Zenith II Extreme Alpha (TRX40) Motherboard Review

The rewards for offering a high-performance flagship motherboard on the TRX40 platform are clear. Vendors are all competing at price points well above �600 which culminates in motherboard options filled to the brim with the features that almost anybody could wish for. ASUS� ROG Zenith II Extreme was no exception to that point. However, ASUS has tak... [PCSTATS]




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ALPHAVILLE 4K

New release: Kino Lorber has announced a new 4k edition of Alphaville! Godard's classic is a wonderful cocktail of detective noir, secret agents, and science fiction. A must see! From the press release: "Kino Lorber have detailed their upcoming 4K Blu-ray release of Jean-Luc Godard's Alphaville (1965), starring Eddie Constantine, Anna Karina, Akim Tamiroff, Michel Delahaye, and Christa Lang. The release is scheduled to arrive on the market on August 13. Synopsis: Government agent Lemmy Caution (Eddie Constantine) is dispatched on a secret mission to Alphaville, a dystopian metropolis in a distant corner of the galaxy. Caution is hot on the trail of rogue agent Henri Dickson (Akim Tamiroff) and a scientist named Von Braun, the creator of Alpha 60, a computer that uses mind control to rule over residents of Alphaville. Caution is aided in his quest to destroy the despotic computer ruler by Von Braun's own daughter, Natacha (Anna Karina).

Special Features and Technical Specs:NEW 4K RESTORATION FROM THE OCN BY STUDIOCANAL (2023)
DOLBY VISION/HDR PRESENTATION OF THE FILM
Audio Commentary by Novelist and Critic Tim Lucas
Anna Karina Interview (4:31)
Colin McCabe Introduction (5:26)
Includes Both Original French and English Audio with Optional English Subtitles
Theatrical Trailer
Limited Edition Reversible Art and O-Card Slipcase
Optional English Subtitles"

More info at Blu-ray


Selected Spy Vibe Posts: Spy Vibe Radio: Dankworth AvengersMancini BookShinobi BluExoticon 2Spy Vibe Radio: Richard DiamondPrisoner figuresBlu ManchuBlu PrisonerByron Janis R.I.P.Spy Vibe Radio: Blake and MortimerChampions PodcastITC BookBond EventBlack Tight Killers BluNew Persuaders BookDavid McCallum R.I.P.Avengers Blu Sets, Spy Vibe Radio: Adventures in ParadiseThe Secret Service bookWorld of GiantsTiki EventsCold War ClassicalPaul at 81007 Comic ExhibitExotikon EventBond 60th EventThe Baron Blu-rayMission: Impossible in 4kJane Bond StripSV Radio: The Man Called FlintstoneLupin III 50thSV Radio: OSS117McCartney 1964Spy Vibe Radio: HunterSpy Vibe Radio: Gao Dalli CID 999Bond Beatles 60thWilliam Klein R.I.P.Spy Vibe Radio: M SquadSpy Vibe Radio: Mr. BroadwayAgent KingSpy Vibe Radio: John KlingSpy Vibe Radio: Unknown Man of ShandigorDanger Man PodcastSpy Vibe Radio: Dr. MabuseBowie DayInterview: Girls Guns GadgetsShandigor BluShag Palm SpringsNew Bond NovelHi-Fi BookJudex Serial BluUFO ComicsInterview: John BussITC Magazine, Interview: Kaiser MarionettesBelmondo R.I.P.007 Corgi EventSpace 1999: The VaultShag Eames LoungeFirecracker ExoticaSpy Vibe Radio: Lola AlbrightTikyaki 5-0Godzilla ScoresMid-Century VillageSpy Vibe radio: Nicola ConteMen's Adventure QuarterlyBilly May FrenesiGary NumanSpy Vader SpyChris Barber LegacyPhantom RetrospectiveAstro-ManSpy Vibe Radio: BatmanJames Bond LexiconRay CathodeSpy Vibe Radio: Johnny StaccatoMatt Helm BluCold War AuctionAvengers Francavilla PrintsAvengers 60th EventIrma Vep BluAvengers Keel DesignRonnie Scott's DocThe Avengers 60th DesignArt of Pan BooksJohn Le Carre R.I.P.Sean Connery R.I.P.New 007 VinylBurke's Law SkaDieter Rams Complete2-Tone DocSpy Vibe Radio: Vendetta Part 2Diana Rigg R.I.P.Moog Micky DolenzBeetle Bailey 70thRSD Spies VinylIan Fleming TributeFellini Box SetSpy Vibe Radio: VendettaThe Saint Podcast BonusThe Saint PodcastBarber Lotus, Trad RootsMorricone R.I.P.Fleetway Spy DesignsJohn Steel CasebooksITC Podcast: The PersuadersDazzle ShipsSpy Vibe Radio: RaumpatrouilleRemembering Richard SalaCrime & Spy Jazz booksNuman is FABBruce Lee Blu, RSD Vinyl SpiesJames Bond's DB5UFO CD SetSpy Vibe radio: Phantom AgentsSteranko is Revolutionary!Interview: The Saint I Ain'tDiabolik InterviewNew 007 SongDiabolik FiguresDiabolik SoundsDiabolik Set DesignDiabolik Park RideDanger Diabolik BluCount Arthur StrongHoney West Title CardsBowie DayNeil Innes R.I.P.Claudine Auger R.I.P.OHMSS at 50Italian Job 50th OSTCharles Schulz ModernPaul DesmondPython 50thRandall Hopkirk 50thThunderbirds DayLazenby Returns to MI6Dr. John R.I.P.Spy Vibe Radio: Lupin IIIFull Article


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Muse And Alphabeats Join Forces To Expand Access To Music-Based Mental Training

Alphabeats, pioneers in mental and focus training by fusing music with neurofeedback technology, have teamed up with Muse to bring music-driven mental training to their consumer electroencephalogram (EEG) platform. This partnership lowers the price barrier to a wider spectrum of users, undercutting Alphabeat's current BrainBit headband setup




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Alphabet in Motion

Kelli Anderson is a magician. Alphabet in Motion is an ABC Pop-up Book on how about letters get their shapes. Mad respect for this work of art which took Kelli 5 years to create. Let’s support her.




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Alpha Star Aviation Services, Riyadh RIYADH Saudi Arabia

Saudi Aramco A Fully Integrated Global Petroleum And Chemicals Enterprise Is The State Owned Oil Company Of The Kingdom Of Sa... Awad Basahi, Riyadh, RIYADH, Saudi Arabia




  • Alpha Star Aviation Services


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Google DeepMind releases AlphaFold 3's source code and model weights for academic use, which could accelerate scientific discovery and drug development

Join our daily and weekly newsletters for the latest updates and exclusive content on industry-leading AI coverage. Learn More Google DeepMind has unexpectedly released the source code and model weights of AlphaFold 3 for academic use, marking a significant advance that could accelerate scientific…




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Alphabet games

Write out each letter of the alphabet. Cut them out in squares and tape them to your clothes and body. Call out a letter for your child to peel off of you until they are all gone.





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Mutation of an atypical oxirane oxyanion hole improves regioselectivity of the {alpha}/{beta}-fold epoxide hydrolase Alp1U [Enzymology]

Epoxide hydrolases (EHs) have been characterized and engineered as biocatalysts that convert epoxides to valuable chiral vicinal diol precursors of drugs and bioactive compounds. Nonetheless, the regioselectivity control of the epoxide ring opening by EHs remains challenging. Alp1U is an α/β-fold EH that exhibits poor regioselectivity in the epoxide hydrolysis of fluostatin C (compound 1) and produces a pair of stereoisomers. Herein, we established the absolute configuration of the two stereoisomeric products and determined the crystal structure of Alp1U. A Trp-186/Trp-187/Tyr-247 oxirane oxygen hole was identified in Alp1U that replaced the canonical Tyr/Tyr pair in α/β-EHs. Mutation of residues in the atypical oxirane oxygen hole of Alp1U improved the regioselectivity for epoxide hydrolysis on 1. The single site Y247F mutation led to highly regioselective (98%) attack at C-3 of 1, whereas the double mutation W187F/Y247F resulted in regioselective (94%) nucleophilic attack at C-2. Furthermore, single-crystal X-ray structures of the two regioselective Alp1U variants in complex with 1 were determined. These findings allowed insights into the reaction details of Alp1U and provided a new approach for engineering regioselective epoxide hydrolases.




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Naturally occurring hotspot cancer mutations in G{alpha}13 promote oncogenic signaling [Molecular Bases of Disease]

Heterotrimeric G-proteins are signaling switches broadly divided into four families based on the sequence and functional similarity of their Gα subunits: Gs, Gi/o, Gq/11, and G12/13. Artificial mutations that activate Gα subunits of each of these families have long been known to induce oncogenic transformation in experimental systems. With the advent of next-generation sequencing, activating hotspot mutations in Gs, Gi/o, or Gq/11 proteins have also been identified in patient tumor samples. In contrast, patient tumor-associated G12/13 mutations characterized to date lead to inactivation rather than activation. By using bioinformatic pathway analysis and signaling assays, here we identified cancer-associated hotspot mutations in Arg-200 of Gα13 (encoded by GNA13) as potent activators of oncogenic signaling. First, we found that components of a G12/13-dependent signaling cascade that culminates in activation of the Hippo pathway effectors YAP and TAZ is frequently altered in bladder cancer. Up-regulation of this signaling cascade correlates with increased YAP/TAZ activation transcriptional signatures in this cancer type. Among the G12/13 pathway alterations were mutations in Arg-200 of Gα13, which we validated to promote YAP/TAZ-dependent (TEAD) and MRTF-A/B-dependent (SRE.L) transcriptional activity. We further showed that this mechanism relies on the same RhoGEF-RhoGTPase cascade components that are up-regulated in bladder cancers. Moreover, Gα13 Arg-200 mutants induced oncogenic transformation in vitro as determined by focus formation assays. In summary, our findings on Gα13 mutants establish that naturally occurring hotspot mutations in Gα subunits of any of the four families of heterotrimeric G-proteins are putative cancer drivers.




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Marked reduction in bile acid synthesis in cholesterol 7{alpha}-hydroxylase-deficient mice does not lead to diminished tissue cholesterol turnover or to hypercholesterolemia

Margrit Schwarz
Sep 1, 1998; 39:1833-1843
Articles




alpha

Building better polymerases: Engineering the replication of expanded genetic alphabets [Molecular Biophysics]

DNA polymerases are today used throughout scientific research, biotechnology, and medicine, in part for their ability to interact with unnatural forms of DNA created by synthetic biologists. Here especially, natural DNA polymerases often do not have the “performance specifications” needed for transformative technologies. This creates a need for science-guided rational (or semi-rational) engineering to identify variants that replicate unnatural base pairs (UBPs), unnatural backbones, tags, or other evolutionarily novel features of unnatural DNA. In this review, we provide a brief overview of the chemistry and properties of replicative DNA polymerases and their evolved variants, focusing on the Klenow fragment of Taq DNA polymerase (Klentaq). We describe comparative structural, enzymatic, and molecular dynamics studies of WT and Klentaq variants, complexed with natural or noncanonical substrates. Combining these methods provides insight into how specific amino acid substitutions distant from the active site in a Klentaq DNA polymerase variant (ZP Klentaq) contribute to its ability to replicate UBPs with improved efficiency compared with Klentaq. This approach can therefore serve to guide any future rational engineering of replicative DNA polymerases.




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The structure of a family 110 glycoside hydrolase provides insight into the hydrolysis of {alpha}-1,3-galactosidic linkages in {lambda}-carrageenan and blood group antigens [Enzymology]

α-Linked galactose is a common carbohydrate motif in nature that is processed by a variety of glycoside hydrolases from different families. Terminal Galα1–3Gal motifs are found as a defining feature of different blood group and tissue antigens, as well as the building block of the marine algal galactan λ-carrageenan. The blood group B antigen and linear α-Gal epitope can be processed by glycoside hydrolases in family GH110, whereas the presence of genes encoding GH110 enzymes in polysaccharide utilization loci from marine bacteria suggests a role in processing λ-carrageenan. However, the structure–function relationships underpinning the α-1,3-galactosidase activity within family GH110 remain unknown. Here we focus on a GH110 enzyme (PdGH110B) from the carrageenolytic marine bacterium Pseudoalteromonas distincta U2A. We showed that the enzyme was active on Galα1–3Gal but not the blood group B antigen. X-ray crystal structures in complex with galactose and unhydrolyzed Galα1–3Gal revealed the parallel β-helix fold of the enzyme and the structural basis of its inverting catalytic mechanism. Moreover, an examination of the active site reveals likely adaptations that allow accommodation of fucose in blood group B active GH110 enzymes or, in the case of PdGH110, accommodation of the sulfate groups found on λ-carrageenan. Overall, this work provides insight into the first member of a predominantly marine clade of GH110 enzymes while also illuminating the structural basis of α-1,3-galactoside processing by the family as a whole.




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Calreticulin enhances the secretory trafficking of a misfolded {alpha}-1-antitrypsin [Protein Structure and Folding]

α1-antitrypsin (AAT) regulates the activity of multiple proteases in the lungs and liver. A mutant of AAT (E342K) called ATZ forms polymers that are present at only low levels in the serum and induce intracellular protein inclusions, causing lung emphysema and liver cirrhosis. An understanding of factors that can reduce the intracellular accumulation of ATZ is of great interest. We now show that calreticulin (CRT), an endoplasmic reticulum (ER) glycoprotein chaperone, promotes the secretory trafficking of ATZ, enhancing the media:cell ratio. This effect is more pronounced for ATZ than with AAT and is only partially dependent on the glycan-binding site of CRT, which is generally relevant to substrate recruitment and folding by CRT. The CRT-related chaperone calnexin does not enhance ATZ secretory trafficking, despite the higher cellular abundance of calnexin-ATZ complexes. CRT deficiency alters the distributions of ATZ-ER chaperone complexes, increasing ATZ-BiP binding and inclusion body formation and reducing ATZ interactions with components required for ER-Golgi trafficking, coincident with reduced levels of the protein transport protein Sec31A in CRT-deficient cells. These findings indicate a novel role for CRT in promoting the secretory trafficking of a protein that forms polymers and large intracellular inclusions. Inefficient secretory trafficking of ATZ in the absence of CRT is coincident with enhanced accumulation of ER-derived ATZ inclusion bodies. Further understanding of the factors that control the secretory trafficking of ATZ and their regulation by CRT could lead to new therapies for lung and liver diseases linked to AAT deficiency.




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{alpha}2-Macroglobulin-like protein 1 can conȷugate and inhibit proteases through their hydroxyl groups, because of an enhanced reactivity of its thiol ester [Protein Structure and Folding]

Proteins in the α-macroglobulin (αM) superfamily use thiol esters to form covalent conjugation products upon their proteolytic activation. αM protease inhibitors use theirs to conjugate proteases and preferentially react with primary amines (e.g. on lysine side chains), whereas those of αM complement components C3 and C4B have an increased hydroxyl reactivity that is conveyed by a conserved histidine residue and allows conjugation to cell surface glycans. Human α2-macroglobulin–like protein 1 (A2ML1) is a monomeric protease inhibitor but has the hydroxyl reactivity–conveying histidine residue. Here, we have investigated the role of hydroxyl reactivity in a protease inhibitor by comparing recombinant WT A2ML1 and the A2ML1 H1084N mutant in which this histidine is removed. Both of A2ML1s' thiol esters were reactive toward the amine substrate glycine, but only WT A2ML1 reacted with the hydroxyl substrate glycerol, demonstrating that His-1084 increases the hydroxyl reactivity of A2ML1's thiol ester. Although both A2ML1s conjugated and inhibited thermolysin, His-1084 was required for the conjugation and inhibition of acetylated thermolysin, which lacks primary amines. Using MS, we identified an ester bond formed between a thermolysin serine residue and the A2ML1 thiol ester. These results demonstrate that a histidine-enhanced hydroxyl reactivity can contribute to protease inhibition by an αM protein. His-1084 did not improve A2ML1's protease inhibition at pH 5, indicating that A2ML1's hydroxyl reactivity is not an adaption to its acidic epidermal environment.




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Characterizing human {alpha}-1,6-fucosyltransferase (FUT8) substrate specificity and structural similarities with related fucosyltransferases [Protein Structure and Folding]

Mammalian Asn-linked glycans are extensively processed as they transit the secretory pathway to generate diverse glycans on cell surface and secreted glycoproteins. Additional modification of the glycan core by α-1,6-fucose addition to the innermost GlcNAc residue (core fucosylation) is catalyzed by an α-1,6-fucosyltransferase (FUT8). The importance of core fucosylation can be seen in the complex pathological phenotypes of FUT8 null mice, which display defects in cellular signaling, development, and subsequent neonatal lethality. Elevated core fucosylation has also been identified in several human cancers. However, the structural basis for FUT8 substrate specificity remains unknown.Here, using various crystal structures of FUT8 in complex with a donor substrate analog, and with four distinct glycan acceptors, we identify the molecular basis for FUT8 specificity and activity. The ordering of three active site loops corresponds to an increased occupancy for bound GDP, suggesting an induced-fit folding of the donor-binding subsite. Structures of the various acceptor complexes were compared with kinetic data on FUT8 active site mutants and with specificity data from a library of glycan acceptors to reveal how binding site complementarity and steric hindrance can tune substrate affinity. The FUT8 structure was also compared with other known fucosyltransferases to identify conserved and divergent structural features for donor and acceptor recognition and catalysis. These data provide insights into the evolution of modular templates for donor and acceptor recognition among GT-B fold glycosyltransferases in the synthesis of diverse glycan structures in biological systems.




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CDKN2A/p16INK4a suppresses hepatic fatty acid oxidation through the AMPK{alpha}2-SIRT1-PPAR{alpha} signaling pathway [Metabolism]

In addition to their well-known role in the control of cellular proliferation and cancer, cell cycle regulators are increasingly identified as important metabolic modulators. Several GWAS have identified SNPs near CDKN2A, the locus encoding for p16INK4a (p16), associated with elevated risk for cardiovascular diseases and type-2 diabetes development, two pathologies associated with impaired hepatic lipid metabolism. Although p16 was recently shown to control hepatic glucose homeostasis, it is unknown whether p16 also controls hepatic lipid metabolism. Using a combination of in vivo and in vitro approaches, we found that p16 modulates fasting-induced hepatic fatty acid oxidation (FAO) and lipid droplet accumulation. In primary hepatocytes, p16-deficiency was associated with elevated expression of genes involved in fatty acid catabolism. These transcriptional changes led to increased FAO and were associated with enhanced activation of PPARα through a mechanism requiring the catalytic AMPKα2 subunit and SIRT1, two known activators of PPARα. By contrast, p16 overexpression was associated with triglyceride accumulation and increased lipid droplet numbers in vitro, and decreased ketogenesis and hepatic mitochondrial activity in vivo. Finally, gene expression analysis of liver samples from obese patients revealed a negative correlation between CDKN2A expression and PPARA and its target genes. Our findings demonstrate that p16 represses hepatic lipid catabolism during fasting and may thus participate in the preservation of metabolic flexibility.




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High-throughput and site-specific N-glycosylation analysis of human alpha-1-acid glycoprotein offers a great potential for new biomarker discovery

Toma Keser
Dec 29, 2020; 0:RA120.002433v1-mcp.RA120.002433
Research




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A potential role for the Gsdf-eEF1{alpha} complex in inhibiting germ cell proliferation: A protein-interaction analysis in medaka (Oryzias latipes) from a proteomics perspective

Xinting Zhang
Dec 8, 2020; 0:RA120.002306v1-mcp.RA120.002306
Research




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G{alpha}s directly drives PDZ-RhoGEF signaling to Cdc42 [Cell Biology]

Gα proteins promote dynamic adjustments of cell shape directed by actin-cytoskeleton reorganization via their respective RhoGEF effectors. For example, Gα13 binding to the RGS-homology (RH) domains of several RH-RhoGEFs allosterically activates these proteins, causing them to expose their catalytic Dbl-homology (DH)/pleckstrin-homology (PH) regions, which triggers downstream signals. However, whether additional Gα proteins might directly regulate the RH-RhoGEFs was not known. To explore this question, we first examined the morphological effects of expressing shortened RH-RhoGEF DH/PH constructs of p115RhoGEF/ARHGEF1, PDZ-RhoGEF (PRG)/ARHGEF11, and LARG/ARHGEF12. As expected, the three constructs promoted cell contraction and activated RhoA, known to be downstream of Gα13. Intriguingly, PRG DH/PH also induced filopodia-like cell protrusions and activated Cdc42. This pathway was stimulated by constitutively active Gαs (GαsQ227L), which enabled endogenous PRG to gain affinity for Cdc42. A chemogenetic approach revealed that signaling by Gs-coupled receptors, but not by those coupled to Gi or Gq, enabled PRG to bind Cdc42. This receptor-dependent effect, as well as CREB phosphorylation, was blocked by a construct derived from the PRG:Gαs-binding region, PRG-linker. Active Gαs interacted with isolated PRG DH and PH domains and their linker. In addition, this construct interfered with GαsQ227L's ability to guide PRG's interaction with Cdc42. Endogenous Gs-coupled prostaglandin receptors stimulated PRG binding to membrane fractions and activated signaling to PKA, and this canonical endogenous pathway was attenuated by PRG-linker. Altogether, our results demonstrate that active Gαs can recognize PRG as a novel effector directing its DH/PH catalytic module to gain affinity for Cdc42.




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Fibrillar {alpha}-synuclein toxicity depends on functional lysosomes [Cell Biology]

Neurodegeneration in Parkinson's disease (PD) can be recapitulated in animals by administration of α-synuclein preformed fibrils (PFFs) into the brain. However, the mechanism by which these PFFs induce toxicity is unknown. Iron is implicated in PD pathophysiology, so we investigated whether α-synuclein PFFs induce ferroptosis, an iron-dependent cell death pathway. A range of ferroptosis inhibitors were added to a striatal neuron-derived cell line (STHdhQ7/7 cells), a dopaminergic neuron–derived cell line (SN4741 cells), and WT primary cortical neurons, all of which had been intoxicated with α-synuclein PFFs. Viability was not recovered by these inhibitors except for liproxstatin-1, a best-in-class ferroptosis inhibitor, when used at high doses. High-dose liproxstatin-1 visibly enlarged the area of a cell that contained acidic vesicles and elevated the expression of several proteins associated with the autophagy-lysosomal pathway similarly to the known lysosomal inhibitors, chloroquine and bafilomycin A1. Consistent with high-dose liproxstatin-1 protecting via a lysosomal mechanism, we further de-monstrated that loss of viability induced by α-synuclein PFFs was attenuated by chloroquine and bafilomycin A1 as well as the lysosomal cysteine protease inhibitors, leupeptin, E-64D, and Ca-074-Me, but not other autophagy or lysosomal enzyme inhibitors. We confirmed using immunofluorescence microscopy that heparin prevented uptake of α-synuclein PFFs into cells but that chloroquine did not stop α-synuclein uptake into lysosomes despite impairing lysosomal function and inhibiting α-synuclein toxicity. Together, these data suggested that α-synuclein PFFs are toxic in functional lysosomes in vitro. Therapeutic strategies that prevent α-synuclein fibril uptake into lysosomes may be of benefit in PD.