Your search keyword '"protein folding"' showing total 133,481 results

101. Protein aggregation: A detrimental symptom or an adaptation mechanism?

Author

Lippi, Alice and Krisko, Anita

Subjects

*TYPE 2 diabetes, *PROTEIN folding, *PROTEIN synthesis, *NEURODEGENERATION, *MACHINE parts

Abstract

Protein quality control mechanisms oversee numerous aspects of protein lifetime. From the point of protein synthesis, protein homeostasis machineries take part in folding, solubilization, and/or degradation of impaired proteins. Some proteins follow an alternative path upon loss of their solubility, thus are secluded from the cytosol and form protein aggregates. Protein aggregates differ in their function and composition, rendering protein aggregation a complex phenomenon that continues to receive plenty of attention in the scientific and medical communities. Traditionally, protein aggregates have been associated with aging and a large spectrum of protein folding diseases, such as neurodegenerative diseases, type 2 diabetes, or cataract. However, a body of evidence suggests that they may act as an adaptive mechanism to overcome transient stressful conditions, serving as a sink for the removal of misfolded proteins from the cytosol or storage compartments for machineries required upon stress release. In this review, we present examples and evidence elaborating different possible roles of protein aggregation and discuss their potential roles in stress survival, aging, and disease, as well as possible anti‐aggregation interventions. [ABSTRACT FROM AUTHOR]

Published

2024

102. PrP meets alpha‐synuclein: Molecular mechanisms and implications for disease.

Author

Vieira, Tuane C. R. G., Barros, Caroline A., Domingues, Renato, and Outeiro, Tiago Fleming

Subjects

*ALZHEIMER'S disease, *AMYOTROPHIC lateral sclerosis, *PARKINSON'S disease, *PRION diseases, *NEURODEGENERATION, *PROTEIN folding

Abstract

The discovery of prions has challenged dogmas and has revolutionized our understanding of protein‐misfolding diseases. The concept of self‐propagation via protein conformational changes, originally discovered for the prion protein (PrP), also applies to other proteins that exhibit similar behavior, such as alpha‐synuclein (aSyn), a central player in Parkinson's disease and in other synucleinopathies. aSyn pathology appears to spread from one cell to another during disease progression, and involves the misfolding and aggregation of aSyn. How the transfer of aSyn between cells occurs is still being studied, but one important hypothesis involves receptor‐mediated transport. Interestingly, recent studies indicate that the cellular prion protein (PrPC) may play a crucial role in this process. PrPC has been shown to act as a receptor/sensor for protein aggregates in different neurodegenerative disorders, including Alzheimer's disease and amyotrophic lateral sclerosis. Here, we provide a comprehensive overview of the current state of knowledge regarding the interaction between aSyn and PrPC and discuss its role in synucleinopathies. We examine the properties of PrP and aSyn, including their structure, function, and aggregation. Additionally, we discuss the current understanding of PrPC's role as a receptor/sensor for aSyn aggregates and identify remaining unanswered questions in this area of research. Ultimately, we posit that exploring the interaction between aSyn and PrPC may offer potential treatment options for synucleinopathies. [ABSTRACT FROM AUTHOR]

Published

2024

103. Community‐Science‐ Projekte in der Wissenschaft: Wie Bürger neue Arzneistoffe mitentwickeln.

Author

Ließmann, Fabian, Landsmann, Anja, Rossa, Jan, and Meiler, Jens

Subjects

*PROTEIN engineering, *PROTEIN folding, *CREATIVE ability in science, *LIGANDS (Biochemistry), *SMALL molecules

Abstract

Summary Community science is experiencing a small revolution with many new projects, some of which combine modern computer science with human creativity and games. In FoldIt, players can fold and design proteins, and create suitable ligands for them. In DrugIt they can create small molecules for target structures and thus, gain direct insights into drug development concepts and support the process directly. The best results from the game are analyzed by researchers and might even be published. [ABSTRACT FROM AUTHOR]

Published

2024

104. Microglia contribute to methamphetamine reinforcement and reflect persistent transcriptional and morphological adaptations to the drug.

Author

Vilca, Samara J., Margetts, Alexander V., Höglund, Leon, Fleites, Isabella, Bystrom, Lauren L., Pollock, Tate A., Bourgain-Guglielmetti, Florence, Wahlestedt, Claes, and Tuesta, Luis M.

Subjects

*DRUG-seeking behavior, *METHAMPHETAMINE, *MICROGLIA, *REWARD (Psychology), *PROTEIN folding, *MOLECULAR shapes

Abstract

[Display omitted] • Methamphetamine induces gene expression changes in microglia that vary by phase of self-administration (maintenance; forced abstinence). • Methamphetamine induces morphological changes in microglia consistent with activation. • These transcriptional and morphological changes persist for up to 21 days after final exposure to methamphetamine. • Transcriptional analysis suggests possible involvement of microglia in regulation of neurotransmitter signaling. • PLX5622 treatment ablates microglia and increases methamphetamine-taking. • PLX5622 treatment during 21-day forced abstinence does not affect context-induced methamphetamine-seeking. Methamphetamine use disorder (MUD) is a chronic, relapsing disease that is characterized by repeated drug use despite negative consequences and for which there are currently no FDA-approved cessation therapeutics. Repeated methamphetamine (METH) use induces long-term gene expression changes in brain regions associated with reward processing and drug-seeking behavior, and recent evidence suggests that methamphetamine-induced neuroinflammation may also shape behavioral and molecular responses to the drug. Microglia, the resident immune cells in the brain, are principal drivers of neuroinflammatory responses and contribute to the pathophysiology of substance use disorders. Here, we investigated transcriptional and morphological changes in dorsal striatal microglia in response to methamphetamine-taking and during methamphetamine abstinence, as well as their functional contribution to drug-taking behavior. We show that methamphetamine self-administration induces transcriptional changes associated with protein folding, mRNA processing, immune signaling, and neurotransmission in dorsal striatal microglia. Importantly, many of these transcriptional changes persist through abstinence, a finding supported by morphological analyses. Functionally, we report that microglial ablation increases methamphetamine-taking, possibly involving neuroimmune and neurotransmitter regulation. In contrast, microglial depletion during abstinence does not alter methamphetamine-seeking. Taken together, these results suggest that methamphetamine induces both short and long-term changes in dorsal striatal microglia that contribute to altered drug-taking behavior and may provide valuable insights into the pathophysiology of MUD. [ABSTRACT FROM AUTHOR]

Published

2024

105. Conserved cysteines prevent C‐mannosylation of mucin Cys domains.

Author

Albers, Marco Darius, Tiemann, Birgit, Kaynert, Jonas Till, Pich, Andreas, and Bakker, Hans

Abstract

Mucins are major components of the mucus. Besides the highly O‐glycosylated tandem repeat domains, mucins contain Cys domains (CysDs). CysDs contain conserved disulfide‐forming cysteine residues as well as a WxxW motif. Since this is the consensus sequence for tryptophan C‐mannosylation, mucin CysDs have been suggested to be targets for C‐mannosyltransferases, but this has never been directly shown. Here, we recombinantly expressed human mucin CysDs in Chinese hamster ovary (CHO) cells and analyzed the C‐mannosylation status. Mass spectrometric analysis revealed that the putative C‐mannose site is not or only barely C‐mannosylated. However, mutation of the adjacent cysteine residues enabled C‐mannosylation to occur. In contrast to mucin CysDs, the homologous CysD of human cartilage intermediate layer protein 1 (CILP1) lacks these cysteine residues preceding the WxxW motif. We show that CILP1 CysD is C‐mannosylated, but introducing a cysteine at the −2 position causes this modification to be lost. We thus conclude that the presence of cysteine residues prevents the modification of the WxxW motif in CysDs. [ABSTRACT FROM AUTHOR]

Published

2024

106. Cystic fibrosis hepatobiliary involvement: an update on imaging in diagnosis and monitoring.

Author

Wood, William, Tinich, Treiy, Lazar, Lauren, Schooler, Gary R., and Sathe, Meghana

Subjects

*HEPATIC fibrosis, *MAGNETIC resonance imaging, *PROTEIN folding, *CYSTIC fibrosis, *MEMBRANE proteins

Abstract

Analysis of the liver using imaging for persons with cystic fibrosis (CF) continues to evolve as new medical therapies are developed improving and extending life. In the 2010s, therapies targeted at modulating protein folding became available to those with CF. Therapeutic options have continued to expand, now providing both correction of protein folding and stabilization for most gene mutations that code for the CF transmembrane receptor protein (CFTR). Today, approximately 80% of persons with CF are eligible for highly effective modulator therapy. With these advancements, the impact of CF on the liver has become more complex, adding metabolism of CFTR modulators to intrinsic CF hepatobiliary involvement (CFHBI) and adding not previously appreciated vascular changes within the liver due to increased longevity in persons with CF. A combination of serum biomarkers and imaging is needed to add clarity to the diagnosis and monitoring of the severity of liver disease. A substantial portion of persons with CF will develop at least CFHBI and a subset will develop advanced cystic fibrosis-associated liver disease (aCFLD); therefore, diagnosis and monitoring need to begin in childhood. In this review, we cover the use of and need for imaging, including elastography, ultrasound, and magnetic resonance imaging (MRI), in diagnosing and monitoring CFHBI and its associated complications. [ABSTRACT FROM AUTHOR]

Published

2024

107. A Conformational-Dependent Interdomain Redox Relay at the Core of Protein Disulfide Isomerase Activity.

Author

Melo, Eduardo P., El-Guendouz, Soukaina, Correia, Cátia, Teodoro, Fernando, Lopes, Carlos, and Martel, Paulo J.

Subjects

*PROTEIN disulfide isomerase, *GREEN fluorescent protein, *FLUORESCENT proteins, *PROTEIN folding, *BIOCHEMICAL substrates

Abstract

Aims: Protein disulfide isomerases (PDIs) are a family of chaperones resident in the endoplasmic reticulum (ER). In addition to holdase function, some members catalyze disulfide bond formation and isomerization, a crucial step for native folding and prevention of aggregation of misfolded proteins. PDIs are characterized by an arrangement of thioredoxin-like domains, with the canonical protein disulfide isomerase A1 (PDIA1) organized as four thioredoxin-like domains forming a horseshoe with two active sites, a and a′, at the extremities. We aimed to clarify important aspects underlying the catalytic cycle of PDIA1 in the context of the full pathways of oxidative protein folding operating in the ER. Results: Using two fluorescent redox sensors, redox green fluorescent protein 2 (roGFP2) and HyPer (circularly permutated yellow fluorescent protein containing the regulatory domain of the H2O2-sensing protein OxyR), either unfolded or native, as client substrates, we identified the N-terminal a active site of PDIA1 as the main oxidant of thiols. From there, electrons can flow to the C-terminal a′ active site, with the redox-dependent conformational flexibility of PDIA1 allowing the formation of an interdomain disulfide bond. The a′ active site then acts as a crossing point to redirect electrons to ER downstream oxidases or back to client proteins to reduce scrambled disulfide bonds. Innovation and Conclusions: The two active sites of PDIA1 work cooperatively as an interdomain redox relay mechanism that explains PDIA1 oxidative activity to form native disulfides and PDIA1 reductase activity to resolve scrambled disulfides. This mechanism suggests a new rationale for shutting down oxidative protein folding under ER redox imbalance. Whether it applies to physiological substrates in cells remains to be shown. [ABSTRACT FROM AUTHOR]

Published

2024

108. Sequence, Structure, and Functional Space of Drosophila De Novo Proteins.

Author

Middendorf, Lasse, Iyengar, Bharat Ravi, and Eicholt, Lars A

Subjects

*PROTEIN structure, *CYTOSKELETAL proteins, *AMINO acid sequence, *SEQUENCE spaces, *PROTEIN folding

Abstract

During de novo emergence, new protein coding genes emerge from previously nongenic sequences. The de novo proteins they encode are dissimilar in composition and predicted biochemical properties to conserved proteins. However, functional de novo proteins indeed exist. Both identification of functional de novo proteins and their structural characterization are experimentally laborious. To identify functional and structured de novo proteins in silico, we applied recently developed machine learning based tools and found that most de novo proteins are indeed different from conserved proteins both in their structure and sequence. However, some de novo proteins are predicted to adopt known protein folds, participate in cellular reactions, and to form biomolecular condensates. Apart from broadening our understanding of de novo protein evolution, our study also provides a large set of testable hypotheses for focused experimental studies on structure and function of de novo proteins in Drosophila. [ABSTRACT FROM AUTHOR]

Published

2024

109. mKate2-K67R/R197H—Extra-Bright Red Fluorescent Biomarker of New Generation. X-Ray Structure and Molecular Dynamic Properties.

Author

Goryacheva, E. A., Rossokhin, A. V., Ruchkin, D. A., Bogdanov, A. M., Artemyev, I. V., Pletneva, N. V., and Plenev, V. Z.

Subjects

*MOLECULAR structure, *DIPOLE moments, *FLUORESCENT proteins, *MOLECULAR dynamics, *PROTEIN folding

Abstract

Objective: Cell biology continuously shows the need for new fluorescent tags with advanced properties. The object of our current study is a new genetically encoded monomeric red fluorescent biomarker mKate2-K67R/R197H (λex/λem 579/603 mn), designed from commercial biomarker mKate2 by two R197H/K67R mutations. The mKate2 precursor, a far-red fluorescent protein, is nearly 3-fold brighter than the previously designed mKate. Compared with commercial mKate2, the double mutant mKate2-K67R/R197H (alternative names FusionRed2 and Diogenes) exhibits an additional ~1.6-fold increase in fluorescence brightness and represents the next generation of extra-bright red fluorescent probes offering novel possibilities for fluorescent imaging of proteins in living cells and animals. Methods: The paper presents the results of X-ray and molecular dynamics study of new bright biomarker mKate2-K67R/R197H. Results and Discussion: The three dimensional structure of new advanced red fluorescent biomarker mKate2-K67R/R197H has been studied by X-ray method at 1.5Å resolution supported by molecular dynamics (MD) study The principal structural fold of the protein is an 11-stranded β-barrel. The nearest chromophore environment (≤ 4 Å) comprises 18 tightly packed residues. Conclusions: The MD study showed that the brightness of mKate2-K67R/R197H and its mKate2 precursor correlates with the dipole moments of the amino acid environments of the chromophores. The higher the dipole moment, the higher the brightness of biomarker. [ABSTRACT FROM AUTHOR]

Published

2024

110. Exploring the therapeutic effects of sulforaphane: an in-depth review on endoplasmic reticulum stress modulation across different disease contexts.

Author

Hajimohammadi, Samaneh, Rameshrad, Maryam, and Karimi, Gholamreza

Subjects

*PROTEIN folding, *ORGANOSULFUR compounds, *TREATMENT effectiveness, *CENTRAL nervous system, *BRASSICACEAE

Abstract

The endoplasmic reticulum (ER) is an intracellular organelle that contributes to the folding of proteins and calcium homeostasis. Numerous elements can disrupt its function, leading to the accumulation of proteins that are unfolded or misfolded in the lumen of the ER, a condition that is known as ER stress. This phenomenon can trigger cell death through the activation of apoptosis and inflammation. Glucoraphanin (GRA) is the predominant glucosinolate found in cruciferous vegetables. Various mechanical and biochemical processes activate the enzyme myrosinase, leading to the hydrolysis of glucoraphanin into the bioactive compound sulforaphane. Sulforaphane is an organosulfur compound that belongs to the isothiocyanate group. It possesses a wide range of activities and has shown remarkable potential as an anti-inflammatory, antioxidant, antitumor, and anti-angiogenic substance. Additionally, sulforaphane is resistant to oxidation, has been demonstrated to have low toxicity, and is considered well-tolerable in individuals. These properties make it a valuable natural dietary supplement for research purposes. Sulforaphane has been demonstrated as a potential candidate drug molecule for managing a range of diseases, primarily because of its potent antioxidant, anti-inflammatory, and anti-apoptotic properties, which can be mediated by modulation of ER stress pathways. This review seeks to cover a wealth of data supporting the broad range of protective functions of sulforaphane, improving various diseases, such as cardiovascular, central nervous system, liver, eye, and reproductive diseases, as well as diabetes, cancer, gastroenteritis, and osteoarthritis, through the amelioration of ER stress in both in vivo and in vitro studies. [ABSTRACT FROM AUTHOR]

Published

2024

111. Assessment of the therapeutic potential of Hsp70 activator against prion diseases using in vitro and in vivo models.

Author

Zayed, Mohammed, Yong-Chan Kim, and Byung-Hoon Jeong

Subjects

HEAT shock proteins, PRION diseases, MOLECULAR chaperones, PROTEIN folding, TREATMENT effectiveness

Abstract

Introduction: Prion diseases are deadly neurodegenerative disorders in both animals and humans, causing the destruction of neural tissue and inducing behavioral manifestations. Heat shock proteins (Hsps), act as molecular chaperones by supporting the appropriate folding of proteins and eliminating the misfolded proteins as well as playing a vital role in cell signaling transduction, cell cycle, and apoptosis control. SW02 is a potent activator of Hsp 70 kDa (Hsp70). Methods: In the current study, the protective effects of SW02 against prion protein 106-126 (PrP106-126)-induced neurotoxicity in human neuroblastoma cells (SH-SY5Y) were investigated. In addition, the therapeutic effects of SW02 in ME7 scrapie-infected mice were evaluated. Results: The results showed that SW02 treatment significantly increased Hsp70 mRNA expression levels and Hsp70 ATPase activity (p < 0.01). SW02 also significantly inhibited cytotoxicity and apoptosis induced by PrP106-126 (p < 0.01) and promoted neurite extension. In vivo, intraperitoneal administration of SW02 did not show a statistically significant difference in survival time (p = 0.16); however, the SW02-treated group exhibited a longer survival time of 223.6 ± 6.0 days compared with the untreated control group survival time of 217.6 ± 5.4 days. In addition, SW02 reduced the PrPSc accumulation in ME7 scrapie-infected mice at 5 months post-injection (p < 0.05). A significant difference was not observed in GFAP expression, an astrocyte marker, between the treated and untreated groups. Conclusion: In conclusion, the potential therapeutic role of the Hsp70 activator SW02 was determined in the present study and may be a novel and effective drug to mitigate the pathologies of prion diseases and other neurodegenerative diseases. Further studies using a combination of two pharmacological activators of Hsp70 are required to maximize the effectiveness of each intervention. [ABSTRACT FROM AUTHOR]

Published

2024

112. Learning noise-induced transitions by multi-scaling reservoir computing.

Author

Lin, Zequn, Lu, Zhaofan, Di, Zengru, and Tang, Ying

Subjects

MACHINE learning, RECURRENT neural networks, TIME series analysis, PROTEIN folding, WHITE noise, NOISE

Abstract

Noise is usually regarded as adversarial to extracting effective dynamics from time series, such that conventional approaches usually aim at learning dynamics by mitigating the noisy effect. However, noise can have a functional role in driving transitions between stable states underlying many stochastic dynamics. We find that leveraging a machine learning model, reservoir computing, can learn noise-induced transitions. We propose a concise training protocol with a focus on a pivotal hyperparameter controlling the time scale. The approach is widely applicable, including a bistable system with white noise or colored noise, where it generates accurate statistics of transition time for white noise and specific transition time for colored noise. Instead, the conventional approaches such as SINDy and the recurrent neural network do not faithfully capture stochastic transitions even for the case of white noise. The present approach is also aware of asymmetry of the bistable potential, rotational dynamics caused by non-detailed balance, and transitions in multi-stable systems. For the experimental data of protein folding, it learns statistics of transition time between folded states, enabling us to characterize transition dynamics from a small dataset. The results portend the exploration of extending the prevailing approaches in learning dynamics from noisy time series. In many natural and engineered systems, noise adds challenges for extracting effective dynamics from time series, at the same time it may have a constructive role of driving transitions between stable states. The authors propose a framework based on reservoir computing for learning noise-induced transitions from data. [ABSTRACT FROM AUTHOR]

Published

2024

113. Solving puzzles using knowledge-based automation: biomimicry of human solvers.

Author

Fauzia, Syifa, Chen, Sean, Hsu, Ren-Jung, Chen, Rex, and Chen, Chi-Ming

Subjects

PATTERN recognition systems, BIOMIMICRY, PICTURE puzzles, PUZZLES, PROTEIN folding, COMPUTATIONAL neuroscience

Abstract

The human brain's remarkable efficiency in solving puzzles through pictorial information processing serves as a valuable inspiration for computational puzzle solving. In this study, we present a nucleation algorithm for automated puzzle solving, developed based on statistical analysis of an empirical database. This algorithm effectively solves puzzles by choosing pieces with infrequent and iridescent edges as nucleation centers, followed by the identification of neighboring pieces with high resemblances from the remaining puzzle pieces. For the 8 different pictures examined in this study, both empirical data and computer simulations consistently demonstrate a power-law relationship between solving time and the number of puzzle pieces, with an exponent less than 2. We explain this relationship through the nucleation model and explore how the exponent is influenced by the color pattern of the puzzle picture. Moreover, our investigation of puzzle-solving processes reveals distinct principal pathways, akin to protein folding behavior. Our study contributes to the development of a cognitive model for human puzzle solving and color pattern recognition. [ABSTRACT FROM AUTHOR]

Published

2024

114. Research Progress of In-Situ Technology in Ultra-High Static Pressure Food Processing.

Author

LIN Yingfeng, FU Chao, ZHANG Sinan, YAO Xueshuang, ZHENG Zhenhong, YANG Jiaxin, and JIANG Zhuo

Subjects

STATIC pressure, PHASE transitions, DENATURATION of proteins, PROTEIN folding, FOOD quality

Abstract

Ultra high static pressure processing technology holds promise for food sterilization, improving food quality, and extracting active ingredients. Traditional research typically assesses the analysis of the structure and function of organic matter under high static pressure after pressure release, capturing only irreversible changes occurring during compression. In-situ monitoring under pressure is rarely conducted. Insitu technology provides dynamic insights into sample behavior, offering a deeper understanding of its transformation process. Consequently, recent years have witnessed a surge in-situ studies performed under high pressure. This article reviews the advancement of high-pressure in-situ analysis technology and its application in high static pressure food processing. Key areas covered, include structural changes and phase transition intervals of protein folding and denaturation under high pressure, in-situ investigations into the mechanism of starch gelatinization, microbial in-situ monitoring and the challenges of in-situ technology in food processing. [ABSTRACT FROM AUTHOR]

Published

2024

115. Pseudophosphorylation of single residues of the J‐domain of DNAJA2 regulates the holding/folding balance of the Hsc70 system.

Author

Velasco‐Carneros, Lorea, Bernardo‐Seisdedos, Ganeko, Maréchal, Jean‐Didier, Millet, Oscar, Moro, Fernando, and Muga, Arturo

Abstract

The Hsp70 system is essential for maintaining protein homeostasis and comprises a central Hsp70 and two accessory proteins that belong to the J‐domain protein (JDP) and nucleotide exchange factor families. Posttranslational modifications offer a means to tune the activity of the system. We explore how phosphorylation of specific residues of the J‐domain of DNAJA2, a class A JDP, regulates Hsc70 activity using biochemical and structural approaches. Among these residues, we find that pseudophosphorylation of Y10 and S51 enhances the holding/folding balance of the Hsp70 system, reducing cochaperone collaboration with Hsc70 while maintaining the holding capacity. Truly phosphorylated J domains corroborate phosphomimetic variant effects. Notably, distinct mechanisms underlie functional impacts of these DNAJA2 variants. Pseudophosphorylation of Y10 induces partial disordering of the J domain, whereas the S51E substitution weakens essential DNAJA2‐Hsc70 interactions without a large structural reorganization of the protein. S51 phosphorylation might be class‐specific, as all cytosolic class A human JDPs harbor a phosphorylatable residue at this position. [ABSTRACT FROM AUTHOR]

Published

2024

116. Synonymous and non‐synonymous codon substitutions can alleviate dependence on GroEL for folding.

Author

Reingewertz, Tali Haviv, Ben‐Maimon, Miki, Zafrir, Zohar, Tuller, Tamir, and Horovitz, Amnon

Abstract

The Escherichia coli GroEL/ES chaperonin system facilitates protein folding in an ATP‐driven manner. There are <100 obligate clients of this system in E. coli although GroEL can interact and assist the folding of a multitude of proteins in vitro. It has remained unclear, however, which features distinguish obligate clients from all the other proteins in an E. coli cell. To address this question, we established a system for selecting mutations in mouse dihydrofolate reductase (mDHFR), a GroEL interactor, that diminish its dependence on GroEL for folding. Strikingly, both synonymous and non‐synonymous codon substitutions were found to reduce mDHFR's dependence on GroEL. The non‐synonymous substitutions increase the rate of spontaneous folding whereas computational analysis indicates that the synonymous substitutions appear to affect translation rates at specific sites. [ABSTRACT FROM AUTHOR]

Published

2024

117. Toxicity Evaluation and Transcriptome Analysis of Yellowstripe Goby (Mugilogobius chulae) in Response to 2,7-Dibromocarbazole Exposure during Early Development.

Author

Gao, Caixia, Lai, Suqun, Zeng, Jin, Peng, Ying, and Li, Jianjun

Subjects

ACUTE toxicity testing, AMINO acid metabolism, MARINE fishes, PROTEIN folding, GENETIC regulation

Abstract

Polyhalogenated carbazoles (PHCZs) are a class of nitrogen-containing heterocyclic compounds that are widely distributed throughout the marine environment and sediment. These compounds share structural and toxicity similarities with dioxins. However, our understanding of the toxicological effects of PHCZs on marine organisms and their underlying molecular mechanisms remains limited. In this study, we employed the marine model organism Mugilogobius chulae as the experimental subject and selected 2,7-dibromocarbazole (2,7-DBCZ), a compound known for its high toxicity and detection frequency, to conduct both an acute toxicity test and transcriptome analysis on M. chulae embryos. Our findings revealed that the 96 h median lethal concentration (LC50) of 2,7-DBCZ for M. chulae embryos was 174 μg/L, with a median effective concentration (EC50) resulting in pericardial edema deformity of 88.82 μg/L. Transcriptome analysis revealed significant impacts on various systems in M. chulae embryos following exposure to 2,7-DBCZ, including the sensory, cardiovascular, immune, and endocrine systems. Furthermore, this compound perturbed signaling pathways such as phototransduction, protein folding and processing, amino acid metabolism, lipid transport, and exogenous compound metabolism. Notably, transcript abundance of the CYP1A gene associated with the activation of the AhR signaling pathway, similar to dioxin-like compounds, was 18.18 times higher than that in the control group. This observation suggests that M. chulae embryos mount a stress response when exposed to PHCZs. In summary, this study contributes to our understanding of the toxicological implications of PHCZ in marine fish and offers a theoretical foundation for risk assessment and regulatory frameworks for PHCZs in the marine environment. [ABSTRACT FROM AUTHOR]

Published

2024

118. Potent Immunomodulators Developed from an Unstable Bacterial Metabolite of Vitamin B2 Biosynthesis.

Author

Mak, Jeffrey Y. W., Rivero, Ryan J. D., Hoang, Huy N., Lim, Xin Yi, Deng, Jieru, McWilliam, Hamish E. G., Villadangos, Jose A., McCluskey, James, Corbett, Alexandra J., and Fairlie, David P.

Subjects

*VITAMIN B2, *T cells, *BIOSYNTHESIS, *T cell receptors, *IMMUNOMODULATORS, *ANTIGEN presenting cells, *MOLECULAR recognition, *MICROBIOLOGICAL synthesis

Abstract

Bacterial synthesis of vitamin B2 generates a by‐product, 5‐(2‐oxopropylideneamino)‐d‐ribityl‐aminouracil (5‐OP‐RU), with potent immunological properties in mammals, but it is rapidly degraded in water. This natural product covalently bonds to the key immunological protein MR1 in the endoplasmic reticulum of antigen presenting cells (APCs), enabling MR1 refolding and trafficking to the cell surface, where it interacts with T cell receptors (TCRs) on mucosal associated invariant T lymphocytes (MAIT cells), activating their immunological and antimicrobial properties. Here, we strategically modify this natural product to understand the molecular basis of its recognition by MR1. This culminated in the discovery of new water‐stable compounds with extremely powerful and distinctive immunological functions. We report their capacity to bind MR1 inside APCs, triggering its expression on the cell surface (EC50 17 nM), and their potent activation (EC50 56 pM) or inhibition (IC50 80 nM) of interacting MAIT cells. We further derivatize compounds with diazirine‐alkyne, biotin, or fluorophore (Cy5 or AF647) labels for detecting, monitoring, and studying cellular MR1. Computer modeling casts new light on the molecular mechanism of activation, revealing that potent activators are first captured in a tyrosine‐ and serine‐lined cleft in MR1 via specific pi‐interactions and H‐bonds, before more tightly attaching via a covalent bond to Lys43 in MR1. This chemical study advances our molecular understanding of how bacterial metabolites are captured by MR1, influence cell surface expression of MR1, interact with T cells to induce immunity, and offers novel clues for developing new vaccine adjuvants, immunotherapeutics, and anticancer drugs. [ABSTRACT FROM AUTHOR]

Published

2024

119. Ferroptosis and endoplasmic reticulum stress in rheumatoid arthritis.

Author

Qin Ao, Huan Hu, and Ying Huang

Subjects

ENDOPLASMIC reticulum, CELLULAR control mechanisms, REACTIVE oxygen species, RHEUMATOID arthritis, PROTEIN folding

Abstract

Ferroptosis is an iron-dependent mode of cell death distinct from apoptosis and necrosis. Its mechanisms mainly involve disordered ironmetabolism, lipid peroxide deposition, and an imbalance of the antioxidant system. The endoplasmic reticulum is an organelle responsible for protein folding, lipid metabolism, and Ca2+ regulation in cells. It can be induced to undergo endoplasmic reticulumstress in response to inflammation, oxidative stress, and hypoxia, thereby regulating intracellular environmental homeostasis through unfolded protein responses. It has been reported that ferroptosis and endoplasmic reticulum stress (ERS) have an interaction pathway and jointly regulate cell survival and death. Both have also been reported separately in rheumatoid arthritis (RA)mechanism studies. However, studies on the correlation between ferroptosis and ERS in RA have not been reported so far. Therefore, this paper reviews the current status of studies and the potential correlation between ferroptosis and ERS in RA, aiming to provide a research reference for developing treatments for RA. [ABSTRACT FROM AUTHOR]

Published

2024

120. Structural basis of tRNA recognition by the widespread OB fold.

Author

Umuhire Juru, Aline, Ghirlando, Rodolfo, and Zhang, Jinwei

Subjects

LEPTIN, NUCLEIC acids, PROTEIN folding, GENETIC transcription, GENETIC translation, TRANSFER RNA

Abstract

The widespread oligonucleotide/oligosaccharide-binding (OB)-fold recognizes diverse substrates from sugars to nucleic acids and proteins, and plays key roles in genome maintenance, transcription, translation, and tRNA metabolism. OB-containing bacterial Trbp and yeast Arc1p proteins are thought to recognize the tRNA elbow or anticodon regions. Here we report a 2.6 Å co-crystal structure of Aquifex aeolicus Trbp111 bound to tRNAIle, which reveals that Trbp recognizes tRNAs solely by capturing their 3′ ends. Structural, mutational, and biophysical analyses show that the Trbp/EMAPII-like OB fold precisely recognizes the single-stranded structure, 3′ terminal location, and specific sequence of the 3′ CA dinucleotide — a universal feature of mature tRNAs. Arc1p supplements its OB – tRNA 3′ end interaction with additional contacts that involve an adjacent basic region and the tRNA body. This study uncovers a previously unrecognized mode of tRNA recognition by an ancient protein fold, and provides insights into protein-mediated tRNA aminoacylation, folding, localization, trafficking, and piracy. The widespread OB fold recognizes diverse substrates from sugars to proteins and nucleic acids. Here the authors reveal how a class of OB fold proteins, exemplified by bacterial Trbp and yeast Arc1p, recognize tRNAs by their universal 3′-CCA ends. [ABSTRACT FROM AUTHOR]

Published

2024

121. Producing recombinant proteins in Vibrio natriegens.

Author

Smith, Matthew, Hernández, José Sánchez, Messing, Simon, Ramakrishnan, Nitya, Higgins, Brianna, Mehalko, Jennifer, Perkins, Shelley, Wall, Vanessa E., Grose, Carissa, Frank, Peter H., Cregger, Julia, Le, Phuong Vi, Johnson, Adam, Sherekar, Mukul, Pagonis, Morgan, Drew, Matt, Hong, Min, Widmeyer, Stephanie R. T., Denson, John-Paul, and Snead, Kelly

Subjects

*RECOMBINANT proteins, *PROTEIN expression, *CHO cell, *ESCHERICHIA coli, *CYTOSKELETAL proteins, *BACTERIAL proteins

Abstract

The diversity of chemical and structural attributes of proteins makes it inherently difficult to produce a wide range of proteins in a single recombinant protein production system. The nature of the target proteins themselves, along with cost, ease of use, and speed, are typically cited as major factors to consider in production. Despite a wide variety of alternative expression systems, most recombinant proteins for research and therapeutics are produced in a limited number of systems: Escherichia coli, yeast, insect cells, and the mammalian cell lines HEK293 and CHO. Recent interest in Vibrio natriegens as a new bacterial recombinant protein expression host is due in part to its short doubling time of ≤ 10 min but also stems from the promise of compatibility with techniques and genetic systems developed for E. coli. We successfully incorporated V. natriegens as an additional bacterial expression system for recombinant protein production and report improvements to published protocols as well as new protocols that expand the versatility of the system. While not all proteins benefit from production in V. natriegens, we successfully produced several proteins that were difficult or impossible to produce in E. coli. We also show that in some cases, the increased yield is due to higher levels of properly folded protein. Additionally, we were able to adapt our enhanced isotope incorporation methods for use with V. natriegens. Taken together, these observations and improvements allowed production of proteins for structural biology, biochemistry, assay development, and structure-based drug design in V. natriegens that were impossible and/or unaffordable to produce in E. coli. Highlights: Production of proteins with reduced aggregation compared to E. coli. Optimized protocols for efficiency and protein expression. Improved yield for specific proteins compared to E. coli. [ABSTRACT FROM AUTHOR]

Published

2024

122. The role of the co-chaperone HOP in plant homeostasis during development and stress.

Author

Castellano, M Mar, Muñoz, Alfonso, Okeke, Isabel C, Novo-Uzal, Esther, Toribio, René, and Mangano, Silvina

Subjects

*HOPS, *PROTEIN folding, *HOMEOSTASIS, *HEAT shock proteins, *PLANT development

Abstract

Proteins need to acquire their native structure in order to become fully functional. In specific cases, the active conformation is obtained spontaneously; nevertheless, many proteins need the assistance of chaperones and co-chaperones to be properly folded. These proteins help to maintain protein homeostasis under control conditions and under different stresses. HOP (HSP70–HSP90 organizing protein) is a highly conserved family of co-chaperones that assist HSP70 and HSP90 in the folding of specific proteins. In the last few years, findings in mammals and yeast have revealed novel functions of HOP and re-defined the role of HOP in protein folding. Here, we provide an overview of the most important aspects of HOP regulation and function in other eukaryotes and analyse whether these aspects are conserved in plants. In addition, we highlight the HOP clients described in plants and the role of HOP in plant development and stress response. [ABSTRACT FROM AUTHOR]

Published

2024

123. Cyclophilin inhibition as a strategy for the treatment of human disease.

Author

Stauffer, Winston T., Goodman, Asha Z., and Gallay, Philippe A.

Subjects

CYCLOPHILINS, THERAPEUTICS, PROTEIN folding, CELL communication, VIRAL replication

Abstract

Cyclophilins (Cyps), characterized as peptidyl-prolyl cis-trans isomerases (PPIases), are highly conserved and ubiquitous, playing a crucial role in protein folding and cellular signaling. This review summarizes the biochemical pathways mediated by Cyps, including their involvement in pathological states such as viral replication, inflammation, and cancer progression, to underscore the therapeutic potential of Cyp inhibition. The exploration of Cyp inhibitors (CypI) in this review, particularly non-immunosuppressive cyclosporine A (CsA) derivatives, highlights their significance as therapeutic agents. The structural and functional nuances of CsA derivatives are examined, including their efficacy, mechanism of action, and the balance between therapeutic benefits and off-target effects. The landscape of CypI is evaluated to emphasize the clinical need for targeted approaches to exploit the complex biology of Cyps and to propose future directions for research that may enhance the utility of non-immunosuppressive CsA derivatives in treating diseases where Cyps play a key pathological role. [ABSTRACT FROM AUTHOR]

Published

2024

124. Codon usage bias in yeasts and its correlation with gene expression, growth temperature, and protein structure.

Author

Baeza, Marcelo, Sepulveda, Dionisia, Cifuentes, Víctor, and Alcaíno, Jennifer

Subjects

PROTEIN structure, GENE expression, YEAST, PROTEIN folding, PROTEIN synthesis, GENETIC translation

Abstract

Codon usage bias (CUB) has been described in viruses, prokaryotes, and eukaryotes and has been linked to several cellular and environmental factors, such as the organism's growth temperature, gene expression levels, and regulation of protein synthesis and folding. Most of the studies in this area have been conducted in bacteria and higher eukaryotes, in some cases with different results. In this study, a comparative analysis of CUB in yeasts isolated from cold and template environments was performed in order to evaluate the correlation of CUB with yeast optimal temperature of growth (OTG), gene expression levels, cellular function, and structure of encoded proteins. Among the main findings, highly expressed ORFs tend to have a more similar CUB within and between yeasts, and a direct correlation between codons ending in C and expression level was generally found. A low correspondence between CUB and OTG was observed, with an inverse correlation for some codons ending in C. The clustering of yeasts based on their CUB partially aligns with their OTG, being more consistent for yeasts with lower OTG. In most yeasts, the abundance of preferred codons was generally lower at the 5′ end of ORFs, higher in segments encoding beta strand, lower in segments encoding extracellular and transmembrane regions, and higher in “translation” and “energy metabolism” pathways, especially in highly expressed ORFs. Based on our findings, it is suggested that the abundance and distribution of preferred and non-preferred codons along mRNAs contribute to proper protein folding and functionality by regulating protein synthesis rates, becoming a more important factor under conditions that require faster protein synthesis in yeasts. [ABSTRACT FROM AUTHOR]

Published

2024

125. Prediction of protein secondary structure by the improved TCN-BiLSTM-MHA model with knowledge distillation.

Author

Zhao, Lufei, Li, Jingyi, Zhan, Weiqiang, Jiang, Xuchu, and Zhang, Biao

Subjects

*PROTEIN structure prediction, *DEEP learning, *AMINO acid sequence, *PROTEIN structure, *DRUG development, *PROTEIN folding

Abstract

Secondary structure prediction is a key step in understanding protein function and biological properties and is highly important in the fields of new drug development, disease treatment, bioengineering, etc. Accurately predicting the secondary structure of proteins helps to reveal how proteins are folded and how they function in cells. The application of deep learning models in protein structure prediction is particularly important because of their ability to process complex sequence information and extract meaningful patterns and features, thus significantly improving the accuracy and efficiency of prediction. In this study, a combined model integrating an improved temporal convolutional network (TCN), bidirectional long short-term memory (BiLSTM), and a multi-head attention (MHA) mechanism is proposed to enhance the accuracy of protein prediction in both eight-state and three-state structures. One-hot encoding features and word vector representations of physicochemical properties are incorporated. A significant emphasis is placed on knowledge distillation techniques utilizing the ProtT5 pretrained model, leading to performance improvements. The improved TCN, achieved through multiscale fusion and bidirectional operations, allows for better extraction of amino acid sequence features than traditional TCN models. The model demonstrated excellent prediction performance on multiple datasets. For the TS115, CB513 and PDB (2018–2020) datasets, the prediction accuracy of the eight-state structure of the six datasets in this paper reached 88.2%, 84.9%, and 95.3%, respectively, and the prediction accuracy of the three-state structure reached 91.3%, 90.3%, and 96.8%, respectively. This study not only improves the accuracy of protein secondary structure prediction but also provides an important tool for understanding protein structure and function, which is particularly applicable to resource-constrained contexts and provides a valuable tool for understanding protein structure and function. [ABSTRACT FROM AUTHOR]

Published

2024

126. Long non‐coding RNA‐mediated modulation of endoplasmic reticulum stress under pathological conditions.

Author

Çiftçi, Yusuf Cem, Yurtsever, Yiğit, and Akgül, Bünyamin

Subjects

UNFOLDED protein response, ENDOPLASMIC reticulum, NUCLEIC acids, EVIDENCE gaps, PROTEIN folding

Abstract

Endoplasmic reticulum (ER) stress, which ensues from an overwhelming protein folding capacity, activates the unfolded protein response (UPR) in an effort to restore cellular homeostasis. As ER stress is associated with numerous diseases, it is highly important to delineate the molecular mechanisms governing the ER stress to gain insight into the disease pathology. Long non‐coding RNAs, transcripts with a length of over 200 nucleotides that do not code for proteins, interact with proteins and nucleic acids, fine‐tuning the UPR to restore ER homeostasis via various modes of actions. Dysregulation of specific lncRNAs is implicated in the progression of ER stress‐related diseases, presenting these molecules as promising therapeutic targets. The comprehensive analysis underscores the importance of understanding the nuanced interplay between lncRNAs and ER stress for insights into disease mechanisms. Overall, this review consolidates current knowledge, identifies research gaps and offers a roadmap for future investigations into the multifaceted roles of lncRNAs in ER stress and associated diseases to shed light on their pivotal roles in the pathogenesis of related diseases. [ABSTRACT FROM AUTHOR]

Published

2024

127. Reassessing the exon-foldon correspondence using frustration analysis.

Author

Galpern, Ezequiel A., Jaafari, Hana, Bueno, Carlos, Wolynes, Peter G., and Ferreiro, Diego U.

Subjects

*PROTEIN folding, *AMINO acid sequence, *PROTEIN domains, *FRUSTRATION

Abstract

Protein folding and evolution are intimately linked phenomena. Here, we revisit the concept of exons as potential protein folding modules across a set of 38 abundant and conserved protein families. Taking advantage of genomic exon-intron organization and extensive protein sequence data, we explore exon boundary conservation and assess the foldon-like behavior of exons using energy landscape theoretic measurements. We found deviations in the exon size distribution from exponential decay indicating selection in evolution. We show that when taken together there is a pronounced tendency to independent foldability for segments corresponding to the more conserved exons, supporting the idea of exon-foldon correspondence. While 45% of the families follow this general trend when analyzed individually, there are some families for which other stronger functional determinants, such as preserving frustrated active sites, may be acting. We further develop a systematic partitioning of protein domains using exon boundary hotspots, showing that minimal common exons correspond with uninterrupted alpha and/or beta elements for the majority of the families but not for all of them. [ABSTRACT FROM AUTHOR]

Published

2024

128. LVPocket: integrated 3D global-local information to protein binding pockets prediction with transfer learning of protein structure classification.

Author

Zhou, Ruifeng, Fan, Jing, Li, Sishu, Zeng, Wenjie, Chen, Yilun, Zheng, Xiaoshan, Chen, Hongyang, and Liao, Jun

Subjects

*PROTEIN binding, *PROTEIN structure, *CYTOSKELETAL proteins, *PROTEIN folding, *TRANSFORMER models

Abstract

Background: Previous deep learning methods for predicting protein binding pockets mainly employed 3D convolution, yet an abundance of convolution operations may lead the model to excessively prioritize local information, thus overlooking global information. Moreover, it is essential for us to account for the influence of diverse protein folding structural classes. Because proteins classified differently structurally exhibit varying biological functions, whereas those within the same structural class share similar functional attributes. Results: We proposed LVPocket, a novel method that synergistically captures both local and global information of protein structure through the integration of Transformer encoders, which help the model achieve better performance in binding pockets prediction. And then we tailored prediction models for data of four distinct structural classes of proteins using the transfer learning. The four fine-tuned models were trained on the baseline LVPocket model which was trained on the sc-PDB dataset. LVPocket exhibits superior performance on three independent datasets compared to current state-of-the-art methods. Additionally, the fine-tuned model outperforms the baseline model in terms of performance. Scientific contribution: We present a novel model structure for predicting protein binding pockets that provides a solution for relying on extensive convolutional computation while neglecting global information about protein structures. Furthermore, we tackle the impact of different protein folding structures on binding pocket prediction tasks through the application of transfer learning methods. [ABSTRACT FROM AUTHOR]

Published

2024

129. TIR domains of TLR family-from the cell culture to the protein sample for structural studies.

Author

Lushpa, Vladislav A., Goncharuk, Marina V., Talyzina, Irina A., Arseniev, Alexander S., Bocharov, Eduard V., Mineev, Konstantin S., and Goncharuk, Sergey A.

Subjects

*CYTOSKELETAL proteins, *ESCHERICHIA coli, *PROTEIN folding, *CELL culture, *TOLL-like receptors, *NUCLEAR magnetic resonance spectroscopy

Abstract

Toll-like receptors (TLRs) are key players in the innate immune system. Despite the great efforts in TLR structural biology, today we know the spatial structures of only four human TLR intracellular TIR domains. All of them belong to one of five subfamilies of receptors. One of the main bottlenecks is the high-level production of correctly folded proteins in soluble form. Here we used a rational approach to find the optimal parameters to produce TIR domains of all ten human TLR family members in soluble form in E. coli cells. We showed that dozens of milligrams of soluble His-tagged TLR2/3/6/7TIR and MBP-tagged TLR3/5/7/8TIR can be produced. We also developed the purification protocols and demonstrated by CD and NMR spectroscopy that purified TLR2/3/7TIR demonstrate a structural organization inherent to TIR domains. This illustrates the correct folding of produced proteins and their suitability for further structural and functional investigations. [ABSTRACT FROM AUTHOR]

Published

2024

130. Including the Ensemble of Unstructured Conformations in the Analysis of Protein's Native State by High‐Pressure NMR Spectroscopy.

Author

Berner, Frederic and Kovermann, Michael

Subjects

*NUCLEAR magnetic resonance spectroscopy, *COLD shock proteins, *CHEMICAL shift (Nuclear magnetic resonance), *PROTEIN conformation, *ANALYTICAL chemistry, *PROTEIN analysis

Abstract

The analysis of pressure induced changes in the chemical shift of proteins allows statements on structural fluctuations proteins exhibit at ambient pressure. The inherent issue of separating general pressure effects from structural related effects on the pressure dependence of chemical shifts has so far been addressed by considering the characteristics of random coil peptides on increasing pressure. In this work, chemically and pressure denatured states of the cold shock protein B from Bacillus subtilis (BsCspB) have been assigned in 2D 1H‐15N HSQC NMR spectra and their dependence on increasing hydrostatic pressure has been evaluated. The pressure denatured polypeptide chain has been used to separate general from structural related effects on 1H and 15N chemical shifts of native BsCspB and the implications on the interpretation of pressure induced changes in the chemical shift regarding the structure of BsCspB are discussed. It has been found that the ensemble of unstructured conformations of BsCspB shows different responses to increasing pressure than random coil peptides do. Thus, the approach used for considering the general effects that arise when hydrostatic pressure increases changes the structural conclusions that are drawn from high pressure NMR spectroscopic experiments that rely on the analysis of chemical shifts. [ABSTRACT FROM AUTHOR]

Published

2024

131. Clinical efficacy of CFTR modulator therapy in people with cystic fibrosis carrying the I1234V mutation.

Author

Aluma, Bat El Bar, Reiter, Joel, Efrati, Ori, Bezalel, Yael, Keler, Shlomit, Ashkenazi, Moshe, Dagan, Adi, Buchnik, Yael, Sadras, Ido, and Cohen-Cymberknoh, Malena

Subjects

*CYSTIC fibrosis transmembrane conductance regulator, *PSEUDOMONAS diseases, *BODY mass index, *PROTEIN folding, *CYSTIC fibrosis

Abstract

• The I1234V mutation is quite common among Arab-Muslim populations. • This mutation cause defective CFTR protein folding, similar to the F508 del mutation. • Currently, the I1234V mutation is not yet eligible for CFTR modulators. • CFTR modulator therapy resulted in significant clinical improvement. The cystic fibrosis transmembrane conductance regulator (CFTR) mutation I1234V (I1234V, p.Ile1234Val, c.3700A>G), is a missense-mutation that creates a cryptic splice site, with the formation of a protein lacking 6 amino acids, that is misfolded and misprocessed. The in vitro effects of CFTR modulator (CFTRm) therapies on human bronchial cell models and intestinal organoids carrying this mutation are conflicting. The aim of this study was therefore to explore the clinical efficacy of CFTRm in people with cystic fibrosis (pwCF) carrying this mutation. This was a retrospective descriptive study of the clinical records of homozygous and compound heterozygous (none F508del) pwCF, for the I1234V mutation, that received CFTRm. Parameters explored were body mass index (BMI), forced expiratory volume in one second percent predicted (FEV 1 %), lung clearance index (LCI) and quantitative sweat chloride measurements. Mean age was 38.6 ± 14 years (range 21–60). Two subjects were homozygous and five compound heterozygous, with minimal function mutations. Four were pancreatic insufficient and three pancreatic sufficient. The two homozygous subjects received Tezacaftor/Ivacaftor, the remaining Elexacaftor/Tezacaftor/Ivacaftor (ETI); treatment ranged from 6 to 12 months. Mean BMI score increased from 21.7 ± 1.3 to 23.6 ± 2.1 kg/m2 (p = 0.04); FEV 1 (%pred) increased by 20.14±10.2while mean change in FEV 1 in the year prior to CFTRm initiation was -0.14±1.18 (p = 0.0001). Additionally, LCI 2.5% decreased from 18.7 to 14.5 (p = 0.07); sweat chloride decreased from 116±10 to 90±17 mEq/L (p = 0.017) and chronic pseudomonas airway infection was eradicated in one subject. This study supports a clinical benefit for CFTRm therapy in pwCF carrying the I1234V mutation. [ABSTRACT FROM AUTHOR]

Published

2024

132. Low-temperature features of the psychrophilic chaperonin from Pseudoalteromonas haloplanktis.

Author

Hertle, Eva, Ursinus, Astrid, and Martin, Jörg

Abstract

Chaperonins from psychrophilic bacteria have been shown to exist as single-ring complexes. This deviation from the standard double-ring structure has been thought to be a beneficial adaptation to the cold environment. Here we show that Cpn60 from the psychrophile Pseudoalteromonas haloplanktis (Ph) maintains its double-ring structure also in the cold. A strongly reduced ATPase activity keeps the chaperonin in an energy-saving dormant state, until binding of client protein activates it. Ph Cpn60 in complex with co-chaperonin Ph Cpn10 efficiently assists in protein folding up to 55 °C. Moreover, we show that recombinant expression of Ph Cpn60 can provide its host Escherichia coli with improved viability under low temperature growth conditions. These properties of the Ph chaperonin may make it a valuable tool in the folding and stabilization of psychrophilic proteins. [ABSTRACT FROM AUTHOR]

Published

2024

133. Integrated transcriptome and microRNA analysis reveals molecular responses to high-temperature stress in the liver of American shad (Alosa sapidissima).

Author

Liu, Ying, Liang, Zhengyuan, Li, Yulin, Zhu, Wenbin, Feng, Bingbing, Xu, Wei, Fu, Jianjun, Wei, Panpan, Luo, Mingkun, and Dong, Zaijie

Subjects

*GENE expression, *TRANSCRIPTOMES, *FISH reproduction, *FOCAL adhesions, *MICRORNA, *PHYSIOLOGICAL effects of heat, *FISH development, *ENDOPLASMIC reticulum, *PROTEIN folding

Abstract

Background: Fish reproduction, development and growth are directly affected by temperature, investigating the regulatory mechanisms behind high temperature stress is helpful to construct a finer molecular network. In this study, we systematically analyzed the transcriptome and miRNA information of American shad (Alosa sapidissima) liver tissues at different cultivation temperatures of 24 ℃ (Low), 27 ℃ (Mid) and 30 ℃ (High) based on a high-throughput sequencing platform. Results: The results showed that there were 1594 differentially expressed genes (DEGs) and 660 differentially expressed miRNAs (DEMs) in the LowLi vs. MidLi comparison group, 473 DEGs and 84 DEMs in the MidLi vs. HighLi group, 914 DEGs and 442 DEMs in the LowLi vs. HighLi group. These included some important genes and miRNAs such as calr, hsp90b1, hsp70, ssa-miR-125a-3p, ssa-miR-92b-5p, dre-miR-15a-3p and novel-m1018-5p. The DEGs were mainly enriched in the protein folding, processing and export pathways of the endoplasmic reticulum; the target genes of the DEMs were mainly enriched in the focal adhesion pathway. Furthermore, the association analysis revealed that the key genes were mainly enriched in the metabolic pathway. Interestingly, we found a significant increase in the number of genes and miRNAs involved in the regulation of heat stress during the temperature change from 24 °C to 27 °C. In addition, we examined the tissue expression characteristics of some key genes and miRNAs by qPCR, and found that calr, hsp90b1 and dre-miR-125b-2-3p were significantly highly expressed in the liver at 27 ℃, while novel-m0481-5p, ssa-miR-125a-3p, ssa-miR-92b-5p, dre-miR-15a-3p and novel-m1018-5p had the highest expression in the heart at 30℃. Finally, the quantitative expression trends of 10 randomly selected DEGs and 10 DEMs were consistent with the sequencing data, indicating the reliability of the results. Conclusions: In summary, this study provides some fundamental data for subsequent in-depth research into the molecular regulatory mechanisms of A. sapidissima response to heat stress, and for the selective breeding of high temperature tolerant varieties. [ABSTRACT FROM AUTHOR]

Published

2024

134. A novel pathological mutant reveals the role of torsional flexibility in the serpin breach in adoption of an aggregation‐prone intermediate.

Author

Kamuda, Kamila, Ronzoni, Riccardo, Majumdar, Avik, Guan, Fiona H. X., Irving, James A., and Lomas, David A.

Subjects

*CELL analysis, *X-ray crystallography, *ACTIVATION energy, *ENDOPLASMIC reticulum, *POLYMERIZATION

Abstract

Mutants of alpha‐1‐antitrypsin cause the protein to self‐associate and form ordered aggregates ('polymers') that are retained within hepatocytes, resulting in a predisposition to the development of liver disease. The associated reduction in secretion, and for some mutants, impairment of function, leads to a failure to protect lung tissue against proteases released during the inflammatory response and an increased risk of emphysema. We report here a novel deficiency mutation (Gly192Cys), that we name the Sydney variant, identified in a patient in heterozygosity with the Z allele (Glu342Lys). Cellular analysis revealed that the novel variant was mostly retained as insoluble polymers within the endoplasmic reticulum. The basis for this behaviour was investigated using biophysical and structural techniques. The variant showed a 40% reduction in inhibitory activity and a reduced stability as assessed by thermal unfolding experiments. Polymerisation involves adoption of an aggregation‐prone intermediate and paradoxically the energy barrier for transition to this state was increased by 16% for the Gly192Cys variant with respect to the wild‐type protein. However, with activation to the intermediate state, polymerisation occurred at a 3.8‐fold faster rate overall. X‐ray crystallography provided two crystal structures of the Gly192Cys variant, revealing perturbation within the 'breach' region with Cys192 in two different orientations: in one structure it faces towards the hydrophobic core while in the second it is solvent‐exposed. This orientational heterogeneity was confirmed by PEGylation. These data show the critical role of the torsional freedom imparted by Gly192 in inhibitory activity and stability against polymerisation. [ABSTRACT FROM AUTHOR]

Published

2024

135. Atomic Tailoring of Ubiquitin Side Chains Influences E2‐Mediated Ubiquitin Chain Formation.

Author

Song, Haewon, Mikami, Toshiki, Majima, Sohei, and Bode, Jeffrey W.

Subjects

*UBIQUITIN, *UBIQUITIN-conjugating enzymes, *TRANSGLUTAMINASES, *CHEMICAL synthesis, *PROTEIN folding, *BLOCKCHAINS, *UBIQUITINATION

Abstract

Ubiquitin (Ub) is a small, highly conserved protein essential for eukaryotic biology, and is unique in its formation of polyubiquitin chains by conjugation to one of its seven lysine side chains. Here we report that atomic tailoring of Ub side chains – i. e. the insertion, deletion, or replacement of specific atoms – has significant and unexpected consequences on the enzymatic conjugation of Ub oligomers by isopeptide bond formation mediated by E2 conjugating enzymes. These studies employed chemical synthesis and ligation methods to prepare numerous specifically tailored Ub monomers on multi‐milligram scales. While some modifications including N‐terminal acylation and methionine replacement did not affect protein folding or Ub chain formation with Ube2 K, other modifications had a pronounced effect of oligomerization with Ubc13/Mms2. We observed that Ala46Hse mutation obliterates the ability of this Ub monomer to accept another Ub at Lys63 in Ubc13‐mediated conjugations. Exhaustive replacement of all seven lysines with shorter surrogates Orn, Dab, or Dap essentially blocks Ub chain formation, and in the case of Dap, precludes proper folding of the Ub protein. [ABSTRACT FROM AUTHOR]

Published

2024

136. The Temperature Dependence of Hydrogen Bonds Is More Uniform in Stable Proteins: An Analysis of NMR h3JNC' Couplings in Four Different Protein Structures.

Author

Alexandrescu, Andrei T. and Dregni, Aurelio J.

Abstract

Long-range HNCO NMR spectra for proteins show crosspeaks due to 1JNC', 2JNC', 3JNCγ, and h3JNC' couplings. The h3JNC' couplings are transmitted through hydrogen bonds and their sizes are correlated to hydrogen bond lengths. We collected long-range HNCO data at a series of temperatures for four protein structures. P22i and CUS-3i are six-stranded beta-barrel I-domains from phages P22 and CUS-3 that share less than 40% sequence identity. The cis and trans states of the C-terminal domain from pore-forming toxin hemolysin ΙΙ (HlyIIC) arise from the isomerization of a single G404-P405 peptide bond. For P22i and CUS-3i, hydrogen bonds detected by NMR agree with those observed in the corresponding domains from cryoEM structures of the two phages. Hydrogen bond lengths derived from the h3JNC' couplings, however, are poorly conserved between the distantly related CUS-3i and P22i domains and show differences even between the closely related cis and trans state structures of HlyIIC. This is consistent with hydrogen bond lengths being determined by local differences in structure rather than the overall folding topology. With increasing temperature, hydrogen bonds typically show an apparent increase in length that has been attributed to protein thermal expansion. Some hydrogen bonds are invariant with temperature, however, while others show apparent decreases in length, suggesting they become stabilized with increasing temperature. Considering the data for the three proteins in this study and previously published data for ubiquitin and GB3, lowered protein folding stability and cooperativity corresponds with a larger range of temperature responses for hydrogen bonds. This suggests a partial uncoupling of hydrogen bond energetics from global unfolding cooperativity as protein stability decreases. [ABSTRACT FROM AUTHOR]

Published

2024

137. NMR Dynamic View of the Destabilization of WW4 Domain by Chaotropic GdmCl and NaSCN.

Author

Lim, Liang-Zhong and Song, Jianxing

Subjects

*PROTEIN stability, *PROTEIN folding, *DENATURATION of proteins, *PROTEIN conformation, *SPINE

Abstract

GdmCl and NaSCN are two strong chaotropic salts commonly used in protein folding and stability studies, but their microscopic mechanisms remain enigmatic. Here, by CD and NMR, we investigated their effects on conformations, stability, binding and backbone dynamics on ps-ns and µs-ms time scales of a 39-residue but well-folded WW4 domain at salt concentrations ≤200 mM. Up to 200 mM, both denaturants did not alter the tertiary packing of WW4, but GdmCl exerted more severe destabilization than NaSCN. Intriguingly, GdmCl had only weak binding to amide protons, while NaSCN showed extensive binding to both hydrophobic side chains and amide protons. Neither denaturant significantly affected the overall ps-ns backbone dynamics, but they distinctively altered µs-ms backbone dynamics. This study unveils that GdmCl and NaSCN destabilize a protein before the global unfolding occurs with differential binding properties and µs-ms backbone dynamics, implying the absence of a simple correlation between thermodynamic stability and backbone dynamics of WW4 at both ps-ns and µs-ms time scales. [ABSTRACT FROM AUTHOR]

Published

2024

138. A Study on How Conformation Entropy of Attached Macromolecules Drives Polymeric Collapse and Protein Folding.

Author

Popa, Ionel

Subjects

*PROTEIN folding, *RANDOM walks, *HYDROGEN bonding, *MACROMOLECULES, *ENTROPY

Abstract

The conformation of macromolecules attached to a surface is influenced by both their excluded volume and steric forces. Here, self‐avoiding random walk simulations are used to evaluate the occurrence of various conformations as a function of the number of monomeric units to estimate the effect of conformational entropy of a tethered chain. Then, a more realistic scenario is assessed, which can more accurately reproduce the shape of a tethered macromolecule. The simulations presented here confirm that it is more likely for a polymer to undergo a collapse conformation rather than a stretched one, as a collapse conformation can be realized in more different ways. Also, they confirm the "mushroom" shape of polymers close to a surface. From this simple approach, the conformation entropy of a model 100‐unit polymer close to a surface is estimated to contribute with over 129 kBT${{k}_{\mathrm{B}}}T$ toward its collapse. This conformation entropy is higher than that of typical hydrogen bonds and even barriers that keep proteins folded. As such, entropic collapse of macromolecules plays an important role in realizing the mushroom shape of attached polymers and can be the driving force in protein folding, while the polypeptide chain emerges from the ribosome. [ABSTRACT FROM AUTHOR]

Published

2024

139. The three-sided right-handed β-helix is a versatile fold for glycan interactions.

Author

Burnim, Audrey A, Dufault-Thompson, Keith, and Jiang, Xiaofang

Subjects

*CARBOHYDRATE-binding proteins, *GLYCANS, *POLYSACCHARIDES, *HYDROGEN bonding interactions, *CARRIER proteins, *PROTEIN folding

Abstract

Interactions between proteins and glycans are critical to various biological processes. With databases of carbohydrate-interacting proteins and increasing amounts of structural data, the three-sided right-handed β-helix (RHBH) has emerged as a significant structural fold for glycan interactions. In this review, we provide an overview of the sequence, mechanistic, and structural features that enable the RHBH to interact with glycans. The RHBH is a prevalent fold that exists in eukaryotes, prokaryotes, and viruses associated with adhesin and carbohydrate-active enzyme (CAZyme) functions. An evolutionary trajectory analysis on structurally characterized RHBH-containing proteins shows that they likely evolved from carbohydrate-binding proteins with their carbohydrate-degrading activities evolving later. By examining three polysaccharide lyase and three glycoside hydrolase structures, we provide a detailed view of the modes of glycan binding in RHBH proteins. The 3-dimensional shape of the RHBH creates an electrostatically and spatially favorable glycan binding surface that allows for extensive hydrogen bonding interactions, leading to favorable and stable glycan binding. The RHBH is observed to be an adaptable domain capable of being modified with loop insertions and charge inversions to accommodate heterogeneous and flexible glycans and diverse reaction mechanisms. Understanding this prevalent protein fold can advance our knowledge of glycan binding in biological systems and help guide the efficient design and utilization of RHBH-containing proteins in glycobiology research. [ABSTRACT FROM AUTHOR]

Published

2024

140. A prospective study of the proteome of equine pre‐implantation embryo.

Author

Teles Filho, Antônio Carlos de A., Sanchez, Deisy J. D., Viana, Arabela G. A., Sheheryar, Sheheryar, Guerreiro, Denise D., Bustamante‐Filho, Ivan C., Martins, Aline M. A., Sousa, Marcelo V., Ricart, Carlos A. O., Fontes, Wagner, and Moura, Arlindo A.

Subjects

*EMBRYOS, *HUMAN embryo transfer, *FERTILIZATION in vitro, *LONGITUDINAL method, *IN vitro studies, *BLASTOCYST, *PROTEOMICS, *MASS spectrometry, *PROTEIN folding

Abstract

The present study was conducted to investigate the global proteome of 8‐day‐old equine blastocysts. Follicular dynamics of eight adult mares were monitored by ultrasonography and inseminated 24 h after the detection of a preovulatory follicle. Four expanded blastocysts were recovered, pooled, and subjected to protein extraction and mass spectrometry. Protein identification was conducted based on four database searches (PEAKS, Proteome Discoverer software, SearchGUI software, and PepExplorer). Enrichment analysis was performed using g:Profiler, Panther, and String platforms. After the elimination of identification redundancies among search tools (at three levels, based on identifiers, peptides, and cross‐database mapping), 1977 proteins were reliably identified in the samples of equine embryos. Proteomic analysis unveiled robust metabolic activity in the 8‐day equine embryo, highlighted by an abundance of proteins engaged in key metabolic pathways like the TCA cycle, ATP biosynthesis, and glycolysis. The prevalence of chaperones among highly abundant proteins suggests that regulation of protein folding, and degradation is a key process during embryo development. These findings pave the way for developing new strategies to improve equine embryo media and optimize in vitro fertilization techniques. [ABSTRACT FROM AUTHOR]

Published

2024

141. Chemical chaperones in metabolic fitness beyond protein folding.

Author

Zito, Ester, Lescure, Alain, and Borgese, Nica

Subjects

*PROTEIN folding, *SMALL molecules, *ENDOPLASMIC reticulum, *INSULIN, *PHENOTYPES

Abstract

Chemical chaperones are small molecules that improve protein folding, alleviating aberrant pathological phenotypes due to protein misfolding. Recent reports suggest that, in parallel with their role in relieving endoplasmic reticulum (ER) stress, chemical chaperones rescue mitochondrial function and insulin signaling. These effects may underlie their pharmacological action on metabolically demanding tissues. [ABSTRACT FROM AUTHOR]

Published

2024

142. Force‐regulated chaperone activity of BiP/ERdj3 is opposite to their homologs DnaK/DnaJ.

Author

Banerjee, Souradeep, Chowdhury, Debojyoti, Chakraborty, Soham, and Haldar, Shubhasis

Abstract

Polypeptide chains experience mechanical tension while translocating through cellular tunnels, which are subsequently folded by molecular chaperones. However, interactions between tunnel‐associated chaperones and these emerging polypeptides under force is not completely understood. Our investigation focused on mechanical chaperone activity of two tunnel‐associated chaperones, BiP and ERdj3 both with and without mechanical constraints and comparing them with their cytoplasmic homologs: DnaK and DnaJ. While BiP/ERdj3 have been observed to exhibit robust foldase activity under force, DnaK/DnaJ showed holdase function. Importantly, the tunnel‐associated chaperones (BiP/ERdj3) transitioned to a holdase state in the absence of force, indicating a force‐dependent chaperone behavior. This chaperone‐driven folding event in the tunnel generated an additional mechanical energy of up to 54 zJ, potentially aiding protein translocation. Our findings align with strain theory, where chaperones with higher intrinsic deformability act as mechanical foldases (BiP, ERdj3), while those with lower deformability serve as holdases (DnaK and DnaJ). This study thus elucidates the differential mechanically regulated chaperoning activity and introduces a novel perspective on co‐translocational protein folding. [ABSTRACT FROM AUTHOR]

Published

2024

143. Mercury: Its role in endoplasmic reticulum stress of pancreatic beta cells in the incident of diabetes mellitus.

Author

Shni, Hazim Mohammed, Hussein, Abdulameer M., and jabber, Sabah N.

Subjects

PANCREATIC beta cells, ENDOPLASMIC reticulum, DIABETES, MERCURY, PROTEIN conformation, INTRACELLULAR calcium, CALCIUM channels, PROTEIN folding

Abstract

Copyright of Revista Latinoamericana de Hipertension is the property of Revista Latinoamericana de Hipertension and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2024

144. Enhancement of protein production in Aspergillus niger by engineering the antioxidant defense metabolism.

Author

Chen, Xin, Pan, Baoxiang, Yu, Leyi, Wang, Bin, and Pan, Li

Subjects

*ASPERGILLUS niger, *TRANSCRIPTION factors, *PROTEIN expression, *PROTEIN folding, *REACTIVE oxygen species

Abstract

Background: Research on protein production holds significant importance in the advancement of food technology, agriculture, pharmaceuticals, and bioenergy. Aspergillus niger stands out as an ideal microbial cell factory for the production of food-grade proteins, owing to its robust protein secretion capacity and excellent safety profile. However, the extensive oxidative folding of proteins within the endoplasmic reticulum (ER) triggers ER stress, consequently leading to protein misfolding reactions. This stressful phenomenon results in the accelerated generation of reactive oxygen species (ROS), thereby inducing oxidative stress. The accumulation of ROS can adversely affect intracellular DNA, proteins, and lipids. Result: In this study, we enhanced the detoxification of ROS in A. niger (SH-1) by integrating multiple modules, including the NADPH regeneration engineering module, the glutaredoxin system, the GSH synthesis engineering module, and the transcription factor module. We assessed the intracellular ROS levels, growth under stress conditions, protein production levels, and intracellular GSH content. Our findings revealed that the overexpression of Glr1 in the glutaredoxin system exhibited significant efficacy across various parameters. Specifically, it reduced the intracellular ROS levels in A. niger by 50%, boosted glucoamylase enzyme activity by 243%, and increased total protein secretion by 88%. Conclusion: The results indicate that moderate modulation of intracellular redox conditions can enhance overall protein output. In conclusion, we present a strategy for augmenting protein production in A. niger and propose a potential approach for optimizing microbial protein production system. [ABSTRACT FROM AUTHOR]

Published

2024

145. The double whammy of ER-retention and dominant-negative effects in numerous autosomal dominant diseases: significance in disease mechanisms and therapy.

Author

Gariballa, Nesrin, Mohamed, Feda, Badawi, Sally, and Ali, Bassam R.

Subjects

*MUTANT proteins, *GENETIC variation, *PROTEIN folding, *PHENOTYPIC plasticity, *PROTEOLYSIS

Abstract

The endoplasmic reticulum (ER) employs stringent quality control mechanisms to ensure the integrity of protein folding, allowing only properly folded, processed and assembled proteins to exit the ER and reach their functional destinations. Mutant proteins unable to attain their correct tertiary conformation or form complexes with their partners are retained in the ER and subsequently degraded through ER-associated protein degradation (ERAD) and associated mechanisms. ER retention contributes to a spectrum of monogenic diseases with diverse modes of inheritance and molecular mechanisms. In autosomal dominant diseases, when mutant proteins get retained in the ER, they can interact with their wild-type counterparts. This interaction may lead to the formation of mixed dimers or aberrant complexes, disrupting their normal trafficking and function in a dominant-negative manner. The combination of ER retention and dominant-negative effects has been frequently documented to cause a significant loss of functional proteins, thereby exacerbating disease severity. This review aims to examine existing literature and provide insights into the impact of dominant-negative effects exerted by mutant proteins retained in the ER in a range of autosomal dominant diseases including skeletal and connective tissue disorders, vascular disorders, neurological disorders, eye disorders and serpinopathies. Most crucially, we aim to emphasize the importance of this area of research, offering substantial potential for understanding the factors influencing phenotypic variability associated with genetic variants. Furthermore, we highlight current and prospective therapeutic approaches targeted at ameliorating the effects of mutations exhibiting dominant-negative effects. These approaches encompass experimental studies exploring treatments and their translation into clinical practice. [ABSTRACT FROM AUTHOR]

Published

2024

146. WTAP and m6A-modified circRNAs modulation during stress response in acute myeloid leukemia progenitor cells.

Author

Iaiza, Alessia, Mazzanti, Gilla, Goeman, Frauke, Cesaro, Bianca, Cortile, Clelia, Corleone, Giacomo, Tito, Claudia, Liccardo, Francesca, De Angelis, Luciana, Petrozza, Vincenzo, Masciarelli, Silvia, Blandino, Giovanni, Fanciulli, Maurizio, Fatica, Alessandro, Fontemaggi, Giulia, and Fazi, Francesco

Subjects

*ACUTE myeloid leukemia, *CIRCULAR RNA, *PROGENITOR cells, *RNA modification & restriction, *OXIDATIVE stress, *PROTEIN folding, *TRIGONOMETRIC functions, *PHYSIOLOGICAL stress

Abstract

N6-methyladenosine (m6A) is one of the most prevalent and conserved RNA modifications. It controls several biological processes, including the biogenesis and function of circular RNAs (circRNAs), which are a class of covalently closed-single stranded RNAs. Several studies have revealed that proteotoxic stress response induction could be a relevant anticancer therapy in Acute Myeloid Leukemia (AML). Furthermore, a strong molecular interaction between the m6A mRNA modification factors and the suppression of the proteotoxic stress response has emerged. Since the proteasome inhibition leading to the imbalance in protein homeostasis is strictly linked to the stress response induction, we investigated the role of Bortezomib (Btz) on m6A regulation and in particular its impact on the modulation of m6A-modified circRNAs expression. Here, we show that treating AML cells with Btz downregulated the expression of the m6A regulator WTAP at translational level, mainly because of increased oxidative stress. Indeed, Btz treatment promoted oxidative stress, with ROS generation and HMOX-1 activation and administration of the reducing agent N-acetylcysteine restored WTAP expression. Additionally, we identified m6A-modified circRNAs modulated by Btz treatment, including circHIPK3, which is implicated in protein folding and oxidative stress regulation. These results highlight the intricate molecular networks involved in oxidative and ER stress induction in AML cells following proteotoxic stress response, laying the groundwork for future therapeutic strategies targeting these pathways. [ABSTRACT FROM AUTHOR]

Published

2024

147. Quantitative proteomics reveals cellular responses to individual mAb expression and tunicamycin in CHO cells.

Author

Sulaj, Eldi, Schwaigerlehner, Linda, Sandell, Felix L., Dohm, Juliane C., Marzban, Gorji, and Kunert, Renate

Subjects

*CHO cell, *TUNICAMYCIN, *UNFOLDED protein response, *PROTEOMICS, *PHARMACEUTICAL biotechnology industry, *PROTEIN folding

Abstract

Chinese hamster ovary (CHO) cells are popular in the pharmaceutical industry for their ability to produce high concentrations of antibodies and their resemblance to human cells in terms of protein glycosylation patterns. Current data indicate the relevance of CHO cells in the biopharmaceutical industry, with a high number of product commendations and a significant market share for monoclonal antibodies. To enhance the production capabilities of CHO cells, a deep understanding of their cellular and molecular composition is crucial. Genome sequencing and proteomic analysis have provided valuable insights into the impact of the bioprocessing conditions, productivity, and product quality. In our investigation, we conducted a comparative analysis of proteomic profiles in high and low monoclonal antibody–producing cell lines and studied the impact of tunicamycin (TM)-induced endoplasmic reticulum (ER) stress. We examined the expression levels of different proteins including unfolded protein response (UPR) target genes by using label-free quantification techniques for protein abundance. Our results show the upregulation of proteins associated with protein folding mechanisms in low producer vs. high producer cell line suggesting a form of ER stress related to specific protein production. Further, Hspa9 and Dnaja3 are notable candidates activated by the mitochondria UPR and play important roles in protein folding processes in mitochondria. We identified significant upregulation of Nedd8 and Lgmn proteins in similar levels which may contribute to UPR stress. Interestingly, the downregulation of Hspa5/Bip and Pdia4 in response to tunicamycin treatment suggests a low-level UPR activation. Key points: • Proteome profiling of recombinant CHO cells under mild TM treatment. • Identified protein clusters are associated with the unfolded protein response (UPR). • The compared cell lines revealed noticeable disparities in protein expression levels. [ABSTRACT FROM AUTHOR]

Published

2024

148. Zinc-finger (ZiF) fold secreted effectors form a functionally diverse family across lineages of the blast fungus Magnaporthe oryzae.

Author

De la Concepcion, Juan Carlos, Langner, Thorsten, Fujisaki, Koki, Yan, Xia, Were, Vincent, Lam, Anson Ho Ching, Saado, Indira, Brabham, Helen J., Win, Joe, Yoshida, Kentaro, Talbot, Nicholas J., Terauchi, Ryohei, Kamoun, Sophien, and Banfield, Mark J.

Subjects

*ZINC-finger proteins, *PYRICULARIA oryzae, *PROTEIN stability, *PHYTOPATHOGENIC microorganisms, *CARRIER proteins, *PROTEIN folding

Abstract

Filamentous plant pathogens deliver effector proteins into host cells to suppress host defence responses and manipulate metabolic processes to support colonization. Understanding the evolution and molecular function of these effectors provides knowledge about pathogenesis and can suggest novel strategies to reduce damage caused by pathogens. However, effector proteins are highly variable, share weak sequence similarity and, although they can be grouped according to their structure, only a few structurally conserved effector families have been functionally characterized to date. Here, we demonstrate that Zinc-finger fold (ZiF) secreted proteins form a functionally diverse effector family in the blast fungus Magnaporthe oryzae. This family relies on the Zinc-finger motif for protein stability and is ubiquitously present in blast fungus lineages infecting 13 different host species, forming different effector tribes. Homologs of the canonical ZiF effector, AVR-Pii, from rice infecting isolates are present in multiple M. oryzae lineages. Wheat infecting strains of the fungus also possess an AVR-Pii like allele that binds host Exo70 proteins and activates the immune receptor Pii. Furthermore, ZiF tribes may vary in the proteins they bind to, indicating functional diversification and an intricate effector/host interactome. Altogether, we uncovered a new effector family with a common protein fold that has functionally diversified in lineages of M. oryzae. This work expands our understanding of the diversity of M. oryzae effectors, the molecular basis of plant pathogenesis and may ultimately facilitate the development of new sources for pathogen resistance. Author summary: Diseases caused by filamentous plant pathogens impact global food production, leading to severe economic and humanitarian consequences. These pathogens secrete hundreds of effectors inside the host to alter cellular processes and to promote infection and disease. Effector proteins have weak or no sequence similarity but can be grouped in structural families based on conserved protein folds. However, very few conserved effector families have been functionally characterized. We have identified a family of effectors with a shared Zinc-finger protein fold (ZiF) that is present in lineages of the blast fungus Magnaporthe oryzae that can, collectively, infect 13 different grasses. We characterized the binding of a sub-set of these proteins to putative Exo70 host targets and showed they can be recognized by the plant immune system. Furthermore, we show that other ZiF effectors do not bind Exo70 targets, suggesting functional specialization within this effector family for alternative interactors. These findings shed light on the diversity of effectors and their molecular functions, as well as potentially leading to the development of new sources of blast disease resistance. [ABSTRACT FROM AUTHOR]

Published

2024

149. High-content analysis of proteostasis capacity in cellular models of amyotrophic lateral sclerosis (ALS).

Author

Lambert-Smith, Isabella A., Shephard, Victoria K., McAlary, Luke, Yerbury, Justin J., and Saunders, Darren N.

Subjects

*AMYOTROPHIC lateral sclerosis, *MUTANT proteins, *GENE expression, *GENETIC variation, *PROTEIN folding, *HOMEOSTASIS, *QUALITY control

Abstract

Disrupted proteome homeostasis (proteostasis) in amyotrophic lateral sclerosis (ALS) has been a major focus of research in the past two decades. However, the proteostasis processes that become disturbed in ALS are not fully understood. Obtaining more detailed knowledge of proteostasis disruption in association with different ALS-causing mutations will improve our understanding of ALS pathophysiology and may identify novel therapeutic targets and strategies for ALS patients. Here we describe the development and use of a novel high-content analysis (HCA) assay to investigate proteostasis disturbances caused by the expression of several ALS-causing gene variants. This assay involves the use of conformationally-destabilised mutants of firefly luciferase (Fluc) to examine protein folding/re-folding capacity in NSC-34 cells expressing ALS-associated mutations in the genes encoding superoxide dismutase-1 (SOD1A4V) and cyclin F (CCNFS621G). We demonstrate that these Fluc isoforms can be used in high-throughput format to report on reductions in the activity of the chaperone network that result from the expression of SOD1A4V, providing multiplexed information at single-cell resolution. In addition to SOD1A4V and CCNFS621G, NSC-34 models of ALS-associated TDP-43, FUS, UBQLN2, OPTN, VCP and VAPB mutants were generated that could be screened using this assay in future work. For ALS-associated mutant proteins that do cause reductions in protein quality control capacity, such as SOD1A4V, this assay has potential to be applied in drug screening studies to identify candidate compounds that can ameliorate this deficiency. [ABSTRACT FROM AUTHOR]

Published

2024

150. Bi-directionalized promoter systems allow methanol-free production of hard-to-express peroxygenases with Komagataella Phaffii.

Author

Besleaga, Mihail, Zimmermann, Christian, Ebner, Katharina, Mach, Robert L., Mach-Aigner, Astrid R., Geier, Martina, Glieder, Anton, Spadiut, Oliver, and Kopp, Julian

Subjects

*PROTEIN disulfide isomerase, *RECOMBINANT proteins, *PROTEIN folding, *PROTEIN expression, *ELECTRON transport

Abstract

Background: Heme-incorporating peroxygenases are responsible for electron transport in a multitude of organisms. Yet their application in biocatalysis is hindered due to their challenging recombinant production. Previous studies suggest Komagataella phaffi to be a suitable production host for heme-containing enzymes. In addition, co-expression of helper proteins has been shown to aid protein folding in yeast. In order to facilitate recombinant protein expression for an unspecific peroxygenase (AnoUPO), we aimed to apply a bi-directionalized expression strategy with Komagataella phaffii. Results: In initial screenings, co-expression of protein disulfide isomerase was found to aid the correct folding of the expressed unspecific peroxygenase in K. phaffi. A multitude of different bi-directionalized promoter combinations was screened. The clone with the most promising promoter combination was scaled up to bioreactor cultivations and compared to a mono-directional construct (expressing only the peroxygenase). The strains were screened for the target enzyme productivity in a dynamic matter, investigating both derepression and mixed feeding (methanol-glycerol) for induction. Set-points from bioreactor screenings, resulting in the highest peroxygenase productivity, for derepressed and methanol-based induction were chosen to conduct dedicated peroxygenase production runs and were analyzed with RT-qPCR. Results demonstrated that methanol-free cultivation is superior over mixed feeding in regard to cell-specific enzyme productivity. RT-qPCR analysis confirmed that mixed feeding resulted in high stress for the host cells, impeding high productivity. Moreover, the bi-directionalized construct resulted in a much higher specific enzymatic activity over the mono-directional expression system. Conclusions: In this study, we demonstrate a methanol-free bioreactor production strategy for an unspecific peroxygenase, yet not shown in literature. Hence, bi-directionalized assisted protein expression in K. phaffii, cultivated under derepressed conditions, is indicated to be an effective production strategy for heme-containing oxidoreductases. This very production strategy might be opening up further opportunities for biocatalysis. [ABSTRACT FROM AUTHOR]

Published

2024