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Author
- Agarwal, Sakshi1
- Ahad, Abdul1
- Ali, Naushad1
- Alvarado, John J1
- Arora, Garima1
- Baksh, Karina A1
- Balskus, Emily P1
- Banerjee, Ruma1
- Bateman, Thomas J1
- Ben Mamoun, Choukri1
- Billot, Raphaël1
- Bradley, Justin M1
- Brown, J Mark1
- Bryant, Donald A1
- Byndloss, Mariana X1
- Bäumler, Andreas J1
- Castellanos, Mildred1
- Cattaneo, Roberto1
- Chabrière, Eric1
- Chaconas, George1
- Chamakura, Karthik1
- Chang, Eugene B1
- Chen, Yumeng1
- Chen, Zhenjun1
- Cho, Seung-Hyun1
Keyword
- microbiology7
- metal homeostasis6
- antibiotic resistance5
- antibiotics5
- bacterial pathogenesis5
- copper5
- gene regulation5
- microbial pathogenesis5
- host-pathogen interaction4
- infectious disease4
- microbiome4
- outer membrane4
- biofilm3
- Escherichia coli (E. coli)3
- metabolomics3
- metalloprotein3
- Mycobacterium tuberculosis3
- natural product3
- peptidoglycan3
- AIDS2
- bacterial genetics2
- bacteriophage2
- Klebsiella pneumonia2
- lipopolysaccharide (LPS)2
- Salmonella enterica2
Microbiology
47 Results
- JBC ReviewsOpen Access
Bacterial iron detoxification at the molecular level
Journal of Biological ChemistryVol. 295Issue 51p17602–17623Published online: December 18, 2020- Justin M. Bradley
- Dimitry A. Svistunenko
- Michael T. Wilson
- Andrew M. Hemmings
- Geoffrey R. Moore
- Nick E. Le Brun
Cited in Scopus: 30Iron is an essential micronutrient, and, in the case of bacteria, its availability is commonly a growth-limiting factor. However, correct functioning of cells requires that the labile pool of chelatable “free” iron be tightly regulated. Correct metalation of proteins requiring iron as a cofactor demands that such a readily accessible source of iron exist, but overaccumulation results in an oxidative burden that, if unchecked, would lead to cell death. The toxicity of iron stems from its potential to catalyze formation of reactive oxygen species that, in addition to causing damage to biological molecules, can also lead to the formation of reactive nitrogen species. - JBC ReviewsOpen Access
The surface lipoproteins of gram-negative bacteria: Protectors and foragers in harsh environments
Journal of Biological ChemistryVol. 296100147Published online: December 9, 2020- Gregory B. Cole
- Thomas J. Bateman
- Trevor F. Moraes
Cited in Scopus: 7Gram-negative pathogens are enveloped by an outer membrane that serves as a double-edged sword: On the one hand, it provides a layer of protection for the bacterium from environmental insults, including other bacteria and the host immune system. On the other hand, it restricts movement of vital nutrients into the cell and provides a plethora of antigens that can be detected by host immune systems. One strategy used to overcome these limitations is the decoration of the outer surface of gram-negative bacteria with proteins tethered to the outer membrane through a lipid anchor. - JBC ReviewsOpen Access
Structure, function, and inhibitor targeting of HIV-1 Nef-effector kinase complexes
Journal of Biological ChemistryVol. 295Issue 44p15158–15171Published online: August 29, 2020- Ryan P. Staudt
- John J. Alvarado
- Lori A. Emert-Sedlak
- Haibin Shi
- Sherry T. Shu
- Thomas E. Wales
- and others
Cited in Scopus: 11Antiretroviral therapy has revolutionized the treatment of AIDS, turning a deadly disease into a manageable chronic condition. Life-long treatment is required because existing drugs do not eradicate HIV-infected cells. The emergence of drug-resistant viral strains and uncertain vaccine prospects highlight the pressing need for new therapeutic approaches with the potential to clear the virus. The HIV-1 accessory protein Nef is essential for viral pathogenesis, making it a promising target for antiretroviral drug discovery. - JBC ReviewsOpen Access
Structure-guided approaches to targeting stress responses in human fungal pathogens
Journal of Biological ChemistryVol. 295Issue 42p14458–14472Published online: August 12, 2020- Emmanuelle V. LeBlanc
- Elizabeth J. Polvi
- Amanda O. Veri
- Gilbert G. Privé
- Leah E. Cowen
Cited in Scopus: 9Fungi inhabit extraordinarily diverse ecological niches, including the human body. Invasive fungal infections have a devastating impact on human health worldwide, killing ∼1.5 million individuals annually. The majority of these deaths are attributable to species of Candida, Cryptococcus, and Aspergillus. Treating fungal infections is challenging, in part due to the emergence of resistance to our limited arsenal of antifungal agents, necessitating the development of novel therapeutic options. Whereas conventional antifungal strategies target proteins or cellular components essential for fungal growth, an attractive alternative strategy involves targeting proteins that regulate fungal virulence or antifungal drug resistance, such as regulators of fungal stress responses. - JBC ReviewsOpen Access
H2S and reactive sulfur signaling at the host-bacterial pathogen interface
Journal of Biological ChemistryVol. 295Issue 38p13150–13168Published online: July 22, 2020- Brenna J.C. Walsh
- David P. Giedroc
Cited in Scopus: 21Bacterial pathogens that cause invasive disease in the vertebrate host must adapt to host efforts to cripple their viability. Major host insults are reactive oxygen and reactive nitrogen species as well as cellular stress induced by antibiotics. Hydrogen sulfide (H2S) is emerging as an important player in cytoprotection against these stressors, which may well be attributed to downstream more oxidized sulfur species termed reactive sulfur species (RSS). In this review, we summarize recent work that suggests that H2S/RSS impacts bacterial survival in infected cells and animals. - JBC ReviewsOpen Access
Engineering acyl-homoserine lactone-interfering enzymes toward bacterial control
Journal of Biological ChemistryVol. 295Issue 37p12993–13007Published online: July 20, 2020- Raphaël Billot
- Laure Plener
- Pauline Jacquet
- Mikael Elias
- Eric Chabrière
- David Daudé
Cited in Scopus: 19Enzymes able to degrade or modify acyl-homoserine lactones (AHLs) have drawn considerable interest for their ability to interfere with the bacterial communication process referred to as quorum sensing. Many proteobacteria use AHL to coordinate virulence and biofilm formation in a cell density–dependent manner; thus, AHL-interfering enzymes constitute new promising antimicrobial candidates. Among these, lactonases and acylases have been particularly studied. These enzymes have been isolated from various bacterial, archaeal, or eukaryotic organisms and have been evaluated for their ability to control several pathogens. - JBC ReviewsOpen Access
How the assembly and protection of the bacterial cell envelope depend on cysteine residues
Journal of Biological ChemistryVol. 295Issue 34p11984–11994Published online: June 2, 2020- Jean-François Collet
- Seung-Hyun Cho
- Bogdan I. Iorga
- Camille V. Goemans
Cited in Scopus: 10The cell envelope of Gram-negative bacteria is a multilayered structure essential for bacterial viability; the peptidoglycan cell wall provides shape and osmotic protection to the cell, and the outer membrane serves as a permeability barrier against noxious compounds in the external environment. Assembling the envelope properly and maintaining its integrity are matters of life and death for bacteria. Our understanding of the mechanisms of envelope assembly and maintenance has increased tremendously over the past two decades. - JBC ReviewsOpen Access
Lipopolysaccharide O-antigens—bacterial glycans made to measure
Journal of Biological ChemistryVol. 295Issue 31p10593–10609Published online: May 18, 2020- Chris Whitfield
- Danielle M. Williams
- Steven D. Kelly
Cited in Scopus: 44Lipopolysaccharides are critical components of bacterial outer membranes. The more conserved lipid A part of the lipopolysaccharide molecule is a major element in the permeability barrier imposed by the outer membrane and offers a pathogen-associated molecular pattern recognized by innate immune systems. In contrast, the long-chain O-antigen polysaccharide (O-PS) shows remarkable structural diversity and fulfills a range of functions, depending on bacterial lifestyles. O-PS production is vital for the success of clinically important Gram-negative pathogens. - JBC ReviewsOpen Access
Translational regulation of environmental adaptation in bacteria
Journal of Biological ChemistryVol. 295Issue 30p10434–10445Published online: June 9, 2020- Rodney Tollerson II
- Michael Ibba
Cited in Scopus: 20Bacteria must rapidly respond to both intracellular and environmental changes to survive. One critical mechanism to rapidly detect and adapt to changes in environmental conditions is control of gene expression at the level of protein synthesis. At each of the three major steps of translation—initiation, elongation, and termination—cells use stimuli to tune translation rate and cellular protein concentrations. For example, changes in nutrient concentrations in the cell can lead to translational responses involving mechanisms such as dynamic folding of riboswitches during translation initiation or the synthesis of alarmones, which drastically alter cell physiology. - JBC ReviewsOpen Access
Malaria parasite plasmepsins: More than just plain old degradative pepsins
Journal of Biological ChemistryVol. 295Issue 25p8425–8441Published online: May 4, 2020- Armiyaw S. Nasamu
- Alexander J. Polino
- Eva S. Istvan
- Daniel E. Goldberg
Cited in Scopus: 24Plasmepsins are a group of diverse aspartic proteases in the malaria parasite Plasmodium. Their functions are strikingly multifaceted, ranging from hemoglobin degradation to secretory organelle protein processing for egress, invasion, and effector export. Some, particularly the digestive vacuole plasmepsins, have been extensively characterized, whereas others, such as the transmission-stage plasmepsins, are minimally understood. Some (e.g. plasmepsin V) have exquisite cleavage sequence specificity; others are fairly promiscuous. - JBC ReviewsOpen Access
Biosynthesis of the modified tetrapyrroles—the pigments of life
Journal of Biological ChemistryVol. 295Issue 20p6888–6925Published online: April 2, 2020- Donald A. Bryant
- C. Neil Hunter
- Martin J. Warren
Cited in Scopus: 99Modified tetrapyrroles are large macrocyclic compounds, consisting of diverse conjugation and metal chelation systems and imparting an array of colors to the biological structures that contain them. Tetrapyrroles represent some of the most complex small molecules synthesized by cells and are involved in many essential processes that are fundamental to life on Earth, including photosynthesis, respiration, and catalysis. These molecules are all derived from a common template through a series of enzyme-mediated transformations that alter the oxidation state of the macrocycle and also modify its size, its side-chain composition, and the nature of the centrally chelated metal ion. - JBC ReviewsOpen Access
Viruses go modular
Journal of Biological ChemistryVol. 295Issue 14p4604–4616Published online: February 28, 2020- Ariel Shepley-McTaggart
- Hao Fan
- Marius Sudol
- Ronald N. Harty
Cited in Scopus: 11The WW domain is a modular protein structure that recognizes the proline-rich Pro-Pro-x-Tyr (PPxY) motif contained in specific target proteins. The compact modular nature of the WW domain makes it ideal for mediating interactions between proteins in complex networks and signaling pathways of the cell (e.g. the Hippo pathway). As a result, WW domains play key roles in a plethora of both normal and disease processes. Intriguingly, RNA and DNA viruses have evolved strategies to hijack cellular WW domain–containing proteins and thereby exploit the modular functions of these host proteins for various steps of the virus life cycle, including entry, replication, and egress. - JBC ReviewsOpen Access
Receptor-mediated cell entry of paramyxoviruses: Mechanisms, and consequences for tropism and pathogenesis
Journal of Biological ChemistryVol. 295Issue 9p2771–2786Published online: January 16, 2020- Chanakha K. Navaratnarajah
- Alex R. Generous
- Iris Yousaf
- Roberto Cattaneo
Cited in Scopus: 33Research in the last decade has uncovered many new paramyxoviruses, airborne agents that cause epidemic diseases in animals including humans. Most paramyxoviruses enter epithelial cells of the airway using sialic acid as a receptor and cause only mild disease. However, others cross the epithelial barrier and cause more severe disease. For some of these viruses, the host receptors have been identified, and the mechanisms of cell entry have been elucidated. The tetrameric attachment proteins of paramyxoviruses have vastly different binding affinities for their cognate receptors, which they contact through different binding surfaces. - JBC ReviewsOpen Access
Uncovering the activities, biological roles, and regulation of bacterial cell wall hydrolases and tailoring enzymes
Journal of Biological ChemistryVol. 295Issue 10p3347–3361Published online: January 23, 2020- Truc Do
- Julia E. Page
- Suzanne Walker
Cited in Scopus: 36Bacteria account for 1000-fold more biomass than humans. They vary widely in shape and size. The morphological diversity of bacteria is due largely to the different peptidoglycan-based cell wall structures that encase bacterial cells. Although the basic structure of peptidoglycan is highly conserved, consisting of long glycan strands that are cross-linked by short peptide chains, the mature cell wall is chemically diverse. Peptidoglycan hydrolases and cell wall–tailoring enzymes that regulate glycan strand length, the degree of cross-linking, and the addition of other modifications to peptidoglycan are central in determining the final architecture of the bacterial cell wall. - JBC ReviewsOpen Access
Changing of the guard: How the Lyme disease spirochete subverts the host immune response
Journal of Biological ChemistryVol. 295Issue 2p301–313Published online: November 21, 2019- George Chaconas
- Mildred Castellanos
- Theodore B. Verhey
Cited in Scopus: 21Lyme disease, also known as Lyme borreliosis, is the most common tick-transmitted disease in the Northern Hemisphere. The disease is caused by the bacterial spirochete Borrelia burgdorferi and other related Borrelia species. One of the many fascinating features of this unique pathogen is an elaborate system for antigenic variation, whereby the sequence of the surface-bound lipoprotein VlsE is continually modified through segmental gene conversion events. This perpetual changing of the guard allows the pathogen to remain one step ahead of the acquired immune response, enabling persistent infection. - JBC ReviewsOpen Access
The manifold roles of microbial ribosomal peptide–based natural products in physiology and ecology
Journal of Biological ChemistryVol. 295Issue 1p34–54Published online: November 29, 2019- Yanyan Li
- Sylvie Rebuffat
Cited in Scopus: 43The ribosomally synthesized and posttranslationally modified peptides (RiPPs), also called ribosomal peptide natural products (RPNPs), form a growing superfamily of natural products that are produced by many different organisms and particularly by bacteria. They are derived from precursor polypeptides whose modification by various dedicated enzymes helps to establish a vast array of chemical motifs. RiPPs have attracted much interest as a source of potential therapeutic agents, and in particular as alternatives to conventional antibiotics to address the bacterial resistance crisis. - JBC ReviewsOpen Access
Allosteric control of metal-responsive transcriptional regulators in bacteria
Journal of Biological ChemistryVol. 295Issue 6p1673–1684Published online: December 19, 2019- Karina A. Baksh
- Deborah B. Zamble
Cited in Scopus: 16Many transition metals are essential trace nutrients for living organisms, but they are also cytotoxic in high concentrations. Bacteria maintain the delicate balance between metal starvation and toxicity through a complex network of metal homeostasis pathways. These systems are coordinated by the activities of metal-responsive transcription factors—also known as metal-sensor proteins or metalloregulators—that are tuned to sense the bioavailability of specific metals in the cell in order to regulate the expression of genes encoding proteins that contribute to metal homeostasis. - MicrobiologyOpen Access
The transcription factor ACE3 controls cellulase activities and lactose metabolism via two additional regulators in the fungus Trichoderma reesei
Journal of Biological ChemistryVol. 294Issue 48p18435–18450Published online: September 9, 2019- Jiajia Zhang
- Yumeng Chen
- Chuan Wu
- Pei Liu
- Wei Wang
- Dongzhi Wei
Cited in Scopus: 32Fungi of the genus Trichoderma are a rich source of enzymes, such as cellulases and hemicellulases, that can degrade lignocellulosic biomass and are therefore of interest for biotechnological approaches seeking to optimize biofuel production. The essential transcription factor ACE3 is involved in cellulase production in Trichoderma reesei; however, the mechanism by which ACE3 regulates cellulase activities is unknown. Here, we discovered that the nominal ace3 sequence in the T. reesei genome available through the Joint Genome Institute is erroneously annotated. - MicrobiologyOpen Access
Double-stranded RNA deaminase ADAR1 promotes the Zika virus replication by inhibiting the activation of protein kinase PKR
Journal of Biological ChemistryVol. 294Issue 48p18168–18180Published online: October 21, 2019- Shili Zhou
- Chao Yang
- Fanfan Zhao
- Yanxia Huang
- Yuxia Lin
- Changbai Huang
- and others
Cited in Scopus: 19Zika virus (ZIKV) is a mosquito-borne flavivirus that has emerged as a threat to global health. The family of adenosine deaminases acting on dsRNA (ADARs) are human host factors important for the genetic diversity and evolution of ZIKV. Here, we further investigated the role of ADAR1 in ZIKV replication by utilizing CRISPR/Cas9-based gene editing and RNAi-based gene knockdown techniques. Both ADAR1 knockout and knockdown significantly reduced ZIKV RNA synthesis, protein levels, and viral titers in several human cell lines. - JBC ReviewsOpen Access
Leveraging a large microbial strain collection for natural product discovery
Journal of Biological ChemistryVol. 294Issue 45p16567–16576Published online: September 30, 2019- Andrew D. Steele
- Christiana N. Teijaro
- Dong Yang
- Ben Shen
Cited in Scopus: 19Throughout history, natural products have significantly contributed to the discovery of novel chemistry, drug leads, and tool molecules to probe and address complex challenges in biology and medicine. Recent microbial genome sequencing efforts have uncovered many microbial biosynthetic gene clusters without an associated natural product. This means that the natural products isolated to date do not fully reflect the biosynthetic potential of microbial strains. This observation has rejuvenated the natural product community and inspired a return to microbial strain collections. - ReviewsOpen Access
Multifaceted HIV integrase functionalities and therapeutic strategies for their inhibition
Journal of Biological ChemistryVol. 294Issue 41p15137–15157Published online: August 29, 2019- Alan N. Engelman
Cited in Scopus: 37Antiretroviral inhibitors that are used to manage HIV infection/AIDS predominantly target three enzymes required for virus replication: reverse transcriptase, protease, and integrase. Although integrase inhibitors were the last among this group to be approved for treating people living with HIV, they have since risen to the forefront of treatment options. Integrase strand transfer inhibitors (INSTIs) are now recommended components of frontline and drug-switch antiretroviral therapy formulations. - JBC ReviewsOpen Access
Trouble is coming: Signaling pathways that regulate general stress responses in bacteria
Journal of Biological ChemistryVol. 294Issue 31p11685–11700Published online: June 13, 2019- Susan Gottesman
Cited in Scopus: 92Bacteria can rapidly and reversibly respond to changing environments via complex transcriptional and post-transcriptional regulatory mechanisms. Many of these adaptations are specific, with the regulatory output tailored to the inducing signal (for instance, repairing damage to cell components or improving acquisition and use of growth-limiting nutrients). However, the general stress response, activated in bacterial cells entering stationary phase or subjected to nutrient depletion or cellular damage, is unique in that its common, broad output is induced in response to many different signals. - THIS ARTICLE HAS BEEN WITHDRAWNOpen Access
Inorganic polyphosphate accumulation suppresses the dormancy response and virulence in Mycobacterium tuberculosis
Journal of Biological ChemistryVol. 294Issue 28p10819–10832Published online: July 1, 2019- Prabhakar Tiwari
- Tannu Priya Gosain
- Mamta Singh
- Gaurav D. Sankhe
- Garima Arora
- Saqib Kidwai
- and others
Cited in Scopus: 11Stringent response pathways involving inorganic polyphosphate (PolyP) play an essential role in bacterial stress adaptation and virulence. The intracellular levels of PolyP are modulated by the activities of polyphosphate kinase-1 (PPK1), polyphosphate kinase-2 (PPK2), and exopolyphosphatases (PPXs). The genome of Mycobacterium tuberculosis encodes two functional PPXs, and simultaneous deletion of ppx1 and ppx2 results in a defect in biofilm formation. We demonstrate here that these PPXs cumulatively contribute to the ability of M. - JBC ReviewsOpen Access
Phage single-gene lysis: Finding the weak spot in the bacterial cell wall
Journal of Biological ChemistryVol. 294Issue 10p3350–3358Published online: November 12, 2018- Karthik Chamakura
- Ry Young
Cited in Scopus: 16In general, the last step in the vegetative cycle of bacterial viruses, or bacteriophages, is lysis of the host. dsDNA phages require multiple lysis proteins, including at least one enzyme that degrades the cell wall (peptidoglycan (PG)). In contrast, the lytic ssDNA and ssRNA phages have a single lysis protein that achieves cell lysis without enzymatically degrading the PG. Here, we review four “single-gene lysis” or Sgl proteins. Three of the Sgls block bacterial cell wall synthesis by binding to and inhibiting several enzymes in the PG precursor pathway. - JBC ReviewsOpen Access
High-resolution studies of lysis–lysogeny decision-making in bacteriophage lambda
Journal of Biological ChemistryVol. 294Issue 10p3343–3349Published online: September 21, 2018- Qiuyan Shao
- Jimmy T. Trinh
- Lanying Zeng
Cited in Scopus: 19Cellular decision-making guides complex development such as cell differentiation and disease progression. Much of our knowledge about decision-making is derived from simple models, such as bacteriophage lambda infection, in which lambda chooses between the vegetative lytic fate and the dormant lysogenic fate. This paradigmatic system is broadly understood but lacking mechanistic details, partly due to limited resolution of past studies. Here, we discuss how modern technologies have enabled high-resolution examination of lambda decision-making to provide new insights and exciting possibilities in studying this classical system.