Publications by authors named "Mika Hirose"

Signal transducer and activator of transcription (STAT) family members mediate signaling in the Janus kinase (JAK)-STAT pathway and are activated by phosphorylation at a conserved tyrosine residue, resulting in dimerization through reciprocal interactions between the phosphotyrosine and a Src homology 2 (SH2) domain. Tyrosine-phosphorylated STAT (pY-STAT) then translocates to the nucleus to induce the expression of genes encoding antiviral proteins. Although the active and functional forms of STATs are conventionally considered to be dimers, STATs can undergo higher-order oligomerization, which is implicated in regulating transcriptional activity.

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Site-2 proteases (S2Ps), conserved intramembrane metalloproteases that maintain cellular homeostasis, are associated with chronic infection and persistence leading to multidrug resistance in bacterial pathogens. A structural model of how S2Ps discriminate and accommodate substrates could help us develop selective antimicrobial agents. We previously proposed that the S2P RseP unwinds helical substrate segments before cleavage, but the mechanism for accommodating a full-length membrane-spanning substrate remained unclear.

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Many bacteria swim in liquid or swarm on surface using the flagellum rotated by a motor driven by specific ion flow. The motor consists of the rotor and stator, and the stator converts the energy of ion flow to mechanical rotation. However, the ion pathway and the mechanism of stator rotation coupled with specific ion flow are still obscure.

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  • Mycobacterium tuberculosis has a thick lipid cell wall that elicits immune responses in humans, primarily through adjuvants acting on innate immune receptors like C-type lectin receptors.
  • Recent research identified trehalose monomycolate (TMM), a major mycobacterial adjuvant, as a trigger for human T cells with a specific unique ɑβTCR, mediated by the antigen-presenting molecule CD1b.
  • TMM-specific T cells are found in non-infected individuals and are more prevalent in active tuberculosis patients, indicating the existence of a pre-formed CD4+ T cell subset that recognizes TMM, suggesting a need to re-evaluate how adjuvants function.
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Messenger RNA vaccines based on lipid nanoparticles (mRNA-LNPs) are promising vaccine modalities. However, mRNA-LNP vaccines frequently cause adverse reactions such as swelling and fever in humans, partly due to the inflammatory nature of LNP. Modification of the ionizable lipids used in LNPs is one approach to avoid these adverse reactions.

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The marine bacterium possesses a polar flagellum driven by a sodium ion flow. The main components of the flagellar motor are the stator and rotor. The C-ring and MS-ring, which are composed of FliG and FliF, respectively, are parts of the rotor.

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Adjuvants are effective tools to enhance vaccine efficacy and control the type of immune responses such as antibody and T helper 1 (Th1)- or Th2-type responses. Several studies suggest that interferon (IFN)-γ-producing Th1 cells play a significant role against infections caused by intracellular bacteria and viruses; however, only a few adjuvants can induce a strong Th1-type immune response. Recently, several studies have shown that lipid nanoparticles (LNPs) can be used as vaccine adjuvants and that each LNP has a different adjuvant activity.

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The 21-residue peptide α3, which is artificially designed and consists of three repeats of 7 residues, is known to rapidly assemble into the α-helix nanofiber. However, its molecular structure within the fiber has not yet been fully elucidated. Thus, we conducted a thorough investigation of the fiber's molecular structure using solid-state NMR and other techniques.

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  • SARS-CoV-2 enters host cells through the spike receptor-binding domain (RBD) interacting with angiotensin-converting enzyme 2 (ACE2).
  • Certain human antibodies targeting the spike N-terminal domain (NTD) can increase ACE2 binding and enhance infection, acting differently than traditional antibody-dependent enhancement mechanisms.
  • The study provides structural models and evidence showing that these NTD-targeting infection-enhancing antibodies (NIEAs) work by crosslinking spike proteins, improving our understanding of their role in SARS-CoV-2 infection.
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  • The Omicron variant of SARS-CoV-2 evolves to evade immunity from vaccines and prior infections, leading to the emergence of subvariants that escape current antibody treatments.
  • An engineered ACE2 decoy shows effectiveness in neutralizing various Omicron subvariants and does not lead to the development of viral escape mutants.
  • Inhalation of aerosolized ACE2 decoys has proven beneficial in rodent models and macaques, suggesting this method could enhance COVID-19 treatment efficacy without invasive procedures.
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α-Synuclein accumulates in Lewy bodies, and this accumulation is a pathological hallmark of Parkinson's disease (PD). Previous studies have indicated a causal role of α-synuclein in the pathogenesis of PD. However, the molecular and cellular mechanisms of α-synuclein toxicity remain elusive.

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Many motile bacteria swim and swarm toward favorable environments using the flagellum, which is rotated by a motor embedded in the inner membrane. The motor is composed of the rotor and the stator, and the motor torque is generated by the change of the interaction between the rotor and the stator induced by the ion flow through the stator. A stator unit consists of two types of membrane proteins termed A and B.

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Prostaglandin receptors have been implicated in a wide range of functions, including inflammation, immune response, reproduction, and cancer. Our group has previously determined the crystal structure of the active-like EP3 bound to its endogenous agonist, prostaglandin E. Here, we present the single-particle cryoelectron microscopy (cryo-EM) structure of the human EP3-G signaling complex at a resolution of 3.

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Site-2 proteases are a conserved family of intramembrane proteases that cleave transmembrane substrates to regulate signal transduction and maintain proteostasis. Here, we elucidated crystal structures of inhibitor-bound forms of bacterial site-2 proteases including RseP. Structure-based chemical modification and cross-linking experiments indicated that the RseP domains surrounding the active center undergo conformational changes to expose the substrate-binding site, suggesting that RseP has a gating mechanism to regulate substrate entry.

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  • Signaling by single-pass transmembrane receptors often leads to the formation of ligand-induced dimers, which can alter receptor function through different conformations.
  • Researchers developed both agonistic and antagonistic receptor dimerizers for PlexinB1 by attaching specific binding peptides to an IgG1 Fc protein, achieving effective modulation of the receptor's activity.
  • Structural analysis indicated that the way these dimerizers organize PlexinB1 directly impacts its signaling ability, highlighting the importance of receptor orientation in dimerization.
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  • The widespread use of antibiotics has led to the emergence of drug-resistant bacteria, requiring new detection methods beyond traditional growth-based approaches.
  • This study focuses on enoxacin-resistant bacteria, using transmission electron microscopy (TEM) images to identify morphological changes without antibiotics.
  • A convolutional neural network (CNN) achieved a high classification accuracy of 0.94, successfully distinguishing between enoxacin-sensitive and resistant strains while highlighting four key genes associated with resistance features.
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Tubulins are critical for the internal organization of eukaryotic cells, and understanding their emergence is an important question in eukaryogenesis. Asgard archaea are the closest known prokaryotic relatives to eukaryotes. Here, we elucidated the apo and nucleotide-bound x-ray structures of an Asgard tubulin from hydrothermal living Odinarchaeota (OdinTubulin).

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In bifidobacteria, phosphoketolase (PKT) plays a key role in the central hexose fermentation pathway called "bifid shunt." The three-dimensional structure of PKT from Bifidobacterium longum with co-enzyme thiamine diphosphate (ThDpp) was determined at 2.1 Å resolution by cryo-EM single-particle analysis using 196,147 particles to build up the structural model of a PKT octamer related by D symmetry.

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  • Desmosine and isodesmosine are important crosslinking amino acids in elastin, which is crucial for the structure of skin.
  • Previous attempts to measure these crosslinkers in human skin have struggled due to the insoluble nature of elastin proteins.
  • This study successfully synthesized isotopically labeled desmosine and used advanced analysis techniques to quantitatively measure desmosine levels in human skin for the first time, detecting approximately 1.43 μg from 1 mg of dry skin.
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Antibodies against the receptor-binding domain (RBD) of the SARS-CoV-2 spike protein prevent SARS-CoV-2 infection. However, the effects of antibodies against other spike protein domains are largely unknown. Here, we screened a series of anti-spike monoclonal antibodies from coronavirus disease 2019 (COVID-19) patients and found that some of antibodies against the N-terminal domain (NTD) induced the open conformation of RBD and thus enhanced the binding capacity of the spike protein to ACE2 and infectivity of SARS-CoV-2.

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Ma'edamines C and D were isolated from an Okinawan marine sponge and exhibited a unique tetrasubstituted pyridinium skeleton. The proposed biosynthetic pathway is similar to that of desmosine and isodesmosine, which are elastin-crosslinking amino acids. In this study, first total synthesis of ma'edamines C and D was achieved via Pr(OTf)-promoted Chichibabin/isoChichibabin pyridinium synthesis starting from the corresponding aldehydes and amine.

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Antibody labeling has been conducted extensively for structure determination using both X-ray crystallography and electron microscopy (EM). However, establishing target-specific antibodies is a prerequisite for applying antibody-assisted structural analysis. To expand the applicability of this strategy, an alternative method has been developed to prepare an antibody complex by inserting an exogenous epitope into the target.

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  • Spermidine acetyltransferase (SAT) from E. coli manages polyamine levels by transferring acetyl groups from acetyl-CoA to spermidine, and its crystal structure was solved at a resolution of 2.5Å.
  • SAT forms a dodecamer structure made of hexameric dimers, with similarities to spermidine/spermine N(1)-acetyltransferase (SSAT), indicating a possible evolutionary relationship, though their polyamine specificities differ.
  • Analysis of the SAT structure and function revealed a unique acetylation mechanism influenced by specific residues, with an acidic cavity playing a critical role in accommodating SPD and CoA for enzyme activity.
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Long-chain fatty acids (FAs) with low water solubility require fatty-acid-binding proteins (FABPs) to transport them from cytoplasm to the mitochondria for energy production. However, the precise mechanism by which these proteins recognize the various lengths of simple alkyl chains of FAs with similar high affinity remains unknown. To address this question, we employed a newly developed calorimetric method for comprehensively evaluating the affinity of FAs, sub-Angstrom X-ray crystallography to accurately determine their 3D structure, and energy calculations of the coexisting water molecules using the computer program WaterMap.

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The bacterial cell-division protein FtsA anchors FtsZ to the cytoplasmic membrane. But how FtsA and FtsZ interact during membrane division remains obscure. We have solved 2.

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