The extra-large cavities of zeolite-like metal-organic frameworks (ZMOFs) offer great potential for their exploration in applications pertinent to larger molecules, like porphyrins. The anionic nature of the framework allowed for facile in situ encapsulation of a cationic free-base porphyrin, and the alpha-cage of our (In-imidazoledicarboxylate)-based rho-ZMOF is ideally suited to the isolation of one porphyrin molecule per cage, which prevents the oxidative self-degradation associated with self-dimerization common in homogeneous catalysis and upon aggregation in solid supports like mesoporous silicates or polymers. The encapsulation of a free-base porphyrin [5,10,15,20-tetrakis(1-methyl-4- pyridinio)porphyrin] and the stability of the rho-ZMOF to metalation conditions, allows for the preparation of a variety of metalloporphyrins (i.e., Mn, Cu, Co, Zn ions) with the ZMOF serving as a platform. The Mn-metallated porphyrin encapsulated in rho-ZMOF shows catalytic activity toward the oxidation of cyclohexane, with turn-over numbers, to the best of our knowledge, higher than reported for similar heterogeneous systems, and our system can be recycled up to 11 cycles, which represents a longer lifetime than reported for any other system.
Two novel porous anionic zeolite-like metal-organic frameworks, rho-ZMOF and sod-ZMOF, have been synthesized by metal-ligand-directed assembly of rigid and directional tetrahedral building units, InN4 synthesized in situ, and doubly deprotonated bis(bidentate) imidazoledicarboxylic acid ligands (HImDC) in the presence of different structure directing agents (SDAs).
Haem-containing proteins such as haemoglobin and myoglobin play an essential role in oxygen transport and storage. Comparison of the amino-acid sequences of globins from Bacteria and Eukarya suggests that they share an early common ancestor, even though the proteins perform different functions in these two kingdoms. Until now, no members of the globin family have been found in the third kingdom, Archaea. Recent studies of biological signalling in the Bacteria and Eukarya have revealed a new class of haem-containing proteins that serve as sensors. Until now, no haem-based sensor has been described in the Archaea. Here we report the first myoglobin-like, haem-containing protein in the Archaea, and the first haem-based aerotactic transducer in the Bacteria (termed HemAT-Hs for the archaeon Halobacterium salinarum, and HemAT-Bs for Bacillus subtilis). These proteins exhibit spectral properties similar to those of myoglobin and trigger aerotactic responses.
It has been demonstrated for the first time that the heme protein cytochrome c (Cyt c) can enter the interior of a MOF despite the larger molecular dimension of the protein relative to the access pore sizes. Mechanistic studies suggest that the Cyt c molecules must undergo a significant conformational change during translocation into the MOF interior through the relatively small nanopores.
A pillared framework formed from 4,4'-bipyridine (bipy) and sheets of dinuclear Cd(2) nodes and 1,4-benzenedicarboxylic acid (bdc) linkers can be prepared in both interpenetrated and noninterpenetrated forms by simply varying the temperature or concentration of the reaction. These results demonstrate that higher temperatures and concentrations favor interpenetration over the corresponding noninterpenetrating structure, an observation that could have broad implications for controlling the synthesis of metal-organic materials.
To carry out essential life processes, nature has had to evolve heme enzymes capable of synthesizing and manipulating complex molecules. These proteins perform a plethora of chemical reactions utilizing a single iron porphyrin active site embedded within an evolutionarily designed protein pocket. We herein report the first class of metal-organic materials (MOMs) that mimic heme enzymes in terms of both structure and reactivity. The MOMzyme-1 class is based upon a prototypal MOM, HKUST-1, into which catalytically active metalloporphyrins are selectively encapsulated in a "ship-in-a-bottle" fashion within one of the three nanoscale cages that exist in HKUST-1. MOMs offer unparalleled levels of permanent porosity and their modular nature affords enormous diversity of structures and properties. The MOMzyme-1 class could therefore represent a new paradigm for heme biomimetic catalysis since it combines the activity of a homogeneous catalyst with the stability and recyclability of heterogeneous catalytic systems within a single material.
SUMMARY Despite the essential functions of Hsp90, little is known about the mechanism that controls substrate entry into its chaperone cycle. We show that the role of Cdc37 cochaperone reaches beyond that of an adaptor protein and find that it participates in the selective recruitment of only client kinases. Cdc37 recognizes kinase specificity determinants in both clients and nonclients and acts as a general kinase scanning factor. Kinase sorting within the client-to-nonclient continuum relies on the ability of Cdc37 to challenge the conformational stability of clients by locally unfolding them. This metastable conformational state has high affinity for Cdc37 and forms stable complexes through a multidomain cochaperone interface. The interaction with nonclients is not accompanied by conformational changes of the substrate and results in substrate dissociation. Collectively, Cdc37 performs a quality control of protein kinases, where induced conformational instability acts as a “flag” for Hsp90 dependence and stable cochaperone association.
The recently discovered prokaryotic signal transducer HemAT, which has been described in both Archaea and Bacteria, mediates aerotactic responses. The N-terminal regions of HemAT from the archaeon Halobacterium salinarum (HemAT-Hs) and from the Gram-positive bacterium Bacillus subtilis (HemAT-Bs) contain a myoglobin-like motif, display characteristic heme-protein absorption spectra, and bind oxygen reversibly. Recombinant HemAT-Hs and HemAT-Bs shorter than 195 and 176 residues, respectively, do not bind heme effectively. Sequence homology comparisons and three-dimensional modeling predict that His-123 is the proximal heme-binding residue in HemAT from both species. The work described here used site-specific mutagenesis and spectroscopy to confirm this prediction, thereby providing direct evidence for a functional domain of prokaryotic signal transducers that bind heme in a globin fold. We postulate that this domain is part of a globin-coupled sensor (GCS) motif that exists as a two-domain transducer having no similarity to the PER-ARNT-SIM (PAS)-domain superfamily transducers. Using the GCS motif, we have identified several two-domain sensors in a variety of prokaryotes. We have cloned, expressed, and purified two potential globin-coupled sensors and performed spectral analysis on them. Both bind heme and show myoglobin-like spectra. This observation suggests that the general function of GCS-type transducers is to bind diatomic oxygen and perhaps other gaseous ligands, and to transmit a conformational signal through a linked signaling domain.proximal histidine ͉ transducer G lobins are heme-containing proteins that are involved in binding and͞or transport of diatomic oxygen. Presently, more than 700 globin sequences are known (1). It has been proposed that all globins have evolved from an ancestral redox protein of about 17 kDa that displayed the globin fold, which is characterized by the presence of eight helices, designated A through H (2). The residues absolutely conserved among all globins are the proximal histidine in the F helix (F8) and phenylalanine in the CD region (CD1) (3, 4). Highly conserved residues include the distal histidine in the E helix (E7), phenylalanine in the CD4 region, and proline at the beginning of the C helix (C2).We recently discovered heme-containing transducers in the archaeon Halobacterium salinarum (HemAT-Hs) and the Grampositive bacterium Bacillus subtilis (HemAT-Bs). These proteins bind diatomic oxygen and mediate an aerotactic response (5). The N termini of these transducers resemble myoglobin, and their C termini are homologous to the cytoplasmic signaling domain of bacterial chemoreceptors. We have also described three-dimensional homology models of the putative oxygensensing domain of HemATs (6). In these models the overall globin topology, including the orientation of the heme prosthetic group, is preserved, as is the hydrophobic core of the hemebinding pocket and the electrostatic stabilization of the CD region. Therefore, an experimental determination of the organizatio...
scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.
hi@scite.ai
334 Leonard St
Brooklyn, NY 11211
Copyright © 2024 scite LLC. All rights reserved.
Made with 💙 for researchers
Part of the Research Solutions Family.