Your search keyword '"STREPTOMYCES"' showing total 6,607 results

1. A dispensable SepIVA orthologue in Streptomyces venezuelae is associated with polar growth and not cell division.

Author

Sen, Beer Chakra, Mavi, Parminder Singh, Irazoki, Oihane, Datta, Susmita, Kaiser, Sebastian, Cava, Felipe, and Flärdh, Klas

Abstract

Background: SepIVA has been reported to be an essential septation factor in Mycolicibacterium smegmatis and Mycobacterium tuberculosis. It is a coiled-coil protein with similarity to DivIVA, a protein necessary for polar growth in members of the phylum Actinomycetota. Orthologues of SepIVA are broadly distributed among actinomycetes, including in Streptomyces spp. Results: To clarify the role of SepIVA and its potential involvement in cell division in streptomycetes, we generated sepIVA deletion mutants in Streptomyces venezuelae and found that sepIVA is dispensable for growth, cell division and sporulation. Further, mNeonGreen-SepIVA fusion protein did not localize at division septa, and we found no evidence of involvement of SepIVA in cell division. Instead, mNeonGreen-SepIVA was accumulated at the tips of growing vegetative hyphae in ways reminiscent of the apical localization of polarisome components like DivIVA. Bacterial two-hybrid system analyses revealed an interaction between SepIVA and DivIVA. The results indicate that SepIVA is associated with polar growth. However, no phenotypic effects of sepIVA deletion could be detected, and no evidence was observed of redundancy with the other DivIVA-like coiled-coil proteins Scy and FilP that are also associated with apical growth in streptomycetes. Conclusions: We conclude that S. venezuelae SepIVA, in contrast to the situation in mycobacteria, is dispensable for growth and viability. The results suggest that it is associated with polar growth rather than septum formation. [ABSTRACT FROM AUTHOR]

Published

2024

2. Streptomyces griseorubens as a microbial cell factory for extracellular uricase production and bioprocess optimization using statistical approach.

Author

El-Naggar, Noura El-Ahmady, El-Ewasy, Sara M., and El-Shweihy, Nancy M.

Abstract

Background: Uricase is a bio-drug used to reduce urate accumulation in gout disease. Thus, there is a continuous demand for screening soil samples derived from a variety of different sources in order to isolate a strain that possesses a high potential for producing uricase. Methods: Streptomyces sp. strain NEAE-5 demonstrated a significant capacity for uricase production was identified based on the physiological, morphological and biochemical characteristics, as well as 16S rDNA sequencing analysis. Using a Plackett–Burman statistical design, the impact of eighteen process factors on uricase production by Streptomyces griseorubens strain NEAE-5 was investigated. Using central composite design, the most important variables that had a favourable positive impact on uricase production by Streptomyces griseorubens strain NEAE-5 were further optimized. Results: It is clear that the morphological and chemotaxonomic features of Streptomyces sp. strain NEAE-5 are typical for the Streptomyces genus. Phylogenetic analysis indicated that Streptomyces sp. strain NEAE-5 belongs to the genus Streptomyces and closely related to Streptomyces griseorubens which it has a 95–96% identity in 16S rDNA gene sequencing. Accordingly, the strain is proposed to be identified as Streptomyces griseorubens strain NEAE-5. The three factors that had the significant positive impacts on uricase production were uric acid, hypoxanthine, and yeast extract. As a result, the best conditions for achieving the highest experimental uricase production by Streptomyces griseorubens strain NEAE-5 after central composite design were (g/L): uric acid 6.96, glycerol 5, hypoxanthine 5.51, MgSO4.7H2O 0.1, KNO3 2, CaCl2 0.5, K2HPO4 0.5, NaCl 0.5, yeast extract 1.08. In addition, the period of incubation is seven days, pH 7.5 and 37 °C with an inoculum size of 2 mL (105 cfu/mL) /100 mL medium. Conclusions: After optimization, the obtained uricase activity was 120.35 U/mL, indicating that the Streptomyces griseorubens strain NEAE-5 is a potent uricase producer and that the statistical approach used for optimization was appropriate. [ABSTRACT FROM AUTHOR]

Published

2024

3. In vitro antimicrobial and antioxidant activities of bioactive compounds extracted from Streptomyces africanus strain E2 isolated from Moroccan soil.

Author

Rammali, Said, Kamal, Fatima Zahra, El Aalaoui, Mohamed, Bencharki, Bouchaib, Burlui, Vasile, khattabi, Abdelkrim, Abderrahim, Aasfar, Saad, Salhi, Romila, Laura, Novac, Bogdan, Aitlhaj-Mhand, Rokaya, Petroaie, Antoneta Dacia, and Ciobică, Alin

Subjects

*PATHOGENIC microorganisms, *KLEBSIELLA pneumoniae, *CINNAMIC acid, *CHLOROGENIC acid, *MULTIDRUG resistance

Abstract

This study aimed to isolate Streptomyces sp. from Moroccan terrestrial ecosystems and identify bioactive compounds through GC–MS analysis. Antimicrobial activity was assessed against various pathogenic microorganisms including Staphylococcus aureus ATCC 25923, Pseudomonas aeruginosa ATCC 27853, Escherichia coli ATCC 25922 and Candida albicans ATCC 60193, and multi-drug resistant strains comprising Listeria monocytogenes, Klebsiella pneumoniae 19K 929, Proteus sp. 19K1313, Klebsiella pneumoniae 20B1572, Proteus vulgaris 16C1737, and Klebsiella pneumoniae 20B1572. Based on the results of the gene sequencing of gene 16S rRNA and phylogenetic analysis, the E2 isolate belongs to the genus Streptomyces with the highest degree of resemblance (97.51%) to the Streptomyces africanus strain NBRC 101005 (NR_112600.1). The isolate exhibited broad-spectrum antibacterial activity, with maximum efficacy against Klebsiella pneumoniae 20B1572 indicated by an inhibition zone diameter of 22.5 ± 0.71mm and a minimum inhibitory concentration (MIC) of 0.0625 mg/mL. The in vitro antioxidant potential of E2 strain was determined through screening of its ethyl acetate extract against sets of antioxidant assays. The results were indicative of E2 strain displaying strong antioxidant activity against ABTS, DPPH free radicals, and FRAP. Furthermore, there was a high significant correlation (p < 0.0001) between the total phenolic and flavonoid content and antioxidant activities. The GC–MS analysis of the extract identified six volatile compounds, with Eugenol (96%) and Maltol (93%) being the most prominent. Additionally, the HPLC–UV/vis analysis revealed six phenolic compounds: gallic acid, chlorogenic acid, vanillic acid, trans-ferulic acid, ellagic acid, and cinnamic acid. Overall, the study highlights Streptomyces sp. strain E2 as a potential source of potent antimicrobial and antioxidant metabolites, offering promise in addressing antibiotic resistance and oxidative stress-related conditions. [ABSTRACT FROM AUTHOR]

Published

2024

4. Machine‐Learning Analysis of Streptomyces coelicolor Transcriptomes Reveals a Transcription Regulatory Network Encompassing Biosynthetic Gene Clusters.

Author

Lee, Yongjae, Choe, Donghui, Palsson, Bernhard O., and Cho, Byung‐Kwan

Subjects

*INDEPENDENT component analysis, *STREPTOMYCES coelicolor, *GENETIC transcription regulation, *GENE regulatory networks, *METABOLITES

Abstract

Streptomyces produces diverse secondary metabolites of biopharmaceutical importance, yet the rate of biosynthesis of these metabolites is often hampered by complex transcriptional regulation. Therefore, a fundamental understanding of transcriptional regulation in Streptomyces is key to fully harness its genetic potential. Here, independent component analysis (ICA) of 454 high‐quality gene expression profiles of the model species Streptomyces coelicolor is performed, of which 249 profiles are newly generated for S. coelicolor cultivated on 20 different carbon sources and 64 engineered strains with overexpressed sigma factors. ICA of the transcriptome dataset reveals 117 independently modulated groups of genes (iModulons), which account for 81.6% of the variance in the dataset. The genes in each iModulon are involved in specific cellular responses, which are often transcriptionally controlled by specific regulators. Also, iModulons accurately predict 25 secondary metabolite biosynthetic gene clusters encoded in the genome. This systemic analysis leads to reveal the functions of previously uncharacterized genes, putative regulons for 40 transcriptional regulators, including 30 sigma factors, and regulation of secondary metabolism via phosphate‐ and iron‐dependent mechanisms in S. coelicolor. ICA of large transcriptomic datasets thus enlightens a new and fundamental understanding of transcriptional regulation of secondary metabolite synthesis along with interconnected metabolic processes in Streptomyces. [ABSTRACT FROM AUTHOR]

Published

2024

5. Improvement of Thermo-Stability and Solvent Tolerant Property of Streptomyces sp. A3301 Lipase by Immobilization Techniques with Application in Poly (lactic acid) Polymerization by Using Biological Process.

Author

Titiporn Panyachanakul, Vichien Kitpreechavanich, Wanlapa Lorliam, and Sukhumaporn Krajangsang

Subjects

*LACTIC acid, *DEGREE of polymerization, *ENZYMES, *MOLECULAR weights, *STREPTOMYCES, *LIPASES

Abstract

The thermo-solvent-tolerant lipase-producing actinomycete, Streptomyces sp. A3301, was utilized as a biocatalyst for poly (lactic acid) or PLA polymerization. The study aimed to optimize lipase immobilization conditions, characterize the immobilized lipase and apply it for PLA polymerization. The results showed using a sponge as the immobilizing matrix was the most effective method, achieving a maximum activity of 277 U/g of sponge. The optimal sponge size was determined to be 0.125 cm³ and pre-soaking the sponge in 0.1 M phosphate buffer at pH 7.0 for 24 h before use proved advantageous. Immobilization significantly enhanced the thermo-stability of the enzyme, with a relative activity ranging from 140 to 190% within the temperature range of 30 to 60 °C. In contrast, the crude lipase exhibited thermo-stability only within the 30 - 50 °C range. The immobilized lipase demonstrated stability under PLA polymerization conditions, which involved a reaction mixture containing toluene and lactic acid and performed at 60 °C for 8 h. The immobilized lipase maintained its activity under this condition for 5 h, retaining a relative activity of 230%, which was 1.2 times higher than the activity of the crude lipase. When the immobilized lipase was used in PLA polymerization, the resulting PLA product exhibited a molecular weight of 5,333 ± 0.02 Da, and the degree of polymerization was approximately 72. These findings underscore the potential of the immobilization technique to enhance lipase activity for PLA polymerization. [ABSTRACT FROM AUTHOR]

Published

2024

6. Flagellar evolution and flagella-independent motility in Actinobacteria.

Author

Chen, Yuanyuan, Zhu, Siqi, Liu, Fan, and Gao, Beile

Subjects

*CELL envelope (Biology), *CELLULAR evolution, *ACTINOBACTERIA, *STREPTOMYCES, *FLAGELLA (Microbiology)

Abstract

Actinobacterial species are mostly thought to be nonmotile. Recent studies have revealed the degenerate evolution of flagella in this phylum and different flagellar rod compositions from the classical model. Moreover, flagella-independent motility by various means has been reported in Streptomyces spp. and Mycobacterium spp., but the underlying mechanisms remain elusive. [ABSTRACT FROM AUTHOR]

Published

2024

7. Harnessing the antagonistic potential and unraveling the bioactive compounds of Streptomyces sp. isolate WAB2 to protect watermelon crop from Colletotrichum orbiculare.

Author

Pradeep, M., Eraivan Arutkani Aiyanathan, Karuppiah, Ayyandurai, M., Kalpana, K., Senthil, K., and Shanthi, Mookiah

Subjects

*WATERMELONS, *PLANT diseases, *BIOLOGICAL pest control agents, *SCANNING electron microscopy, *STREPTOMYCES

Abstract

Watermelon (Citrullus lanatus Thumb) is a significant vegetable crop globally and is prone to anthracnose disease caused by Colletotrichum spp. The use of chemical fungicides for managing crop diseases has adverse impacts on the environment and human health. Therefore, it is important to use biocontrol agents for disease management. In this study, streptomycetes were assessed as a potential biocontrol agent against anthracnose pathogen, Colletotrichum orbiculare WEC2. The potent Streptomyces sp. isolate WAB2 was isolated from healthy watermelon plants and showed remarkable antifungal efficacy against C. orbiculare WEC2. Rigorous assays confirmed its performance against C. orbiculare WEC2. Bioactive compounds produced by Streptomyces sp. isolate WAB2 were identified using Gas Chromatography–Mass Spectrometry (GC–MS). An SEM study indicated the parasitic action of Streptomyces sp. isolate WAB2 against the pathogen. The formulated talc-based product of Streptomyces sp. isolate WAB2 was effective when applied as a seed treatment + foliar spray against C. orbiculare WEC2 under pot culture conditions. These treatments reduced the disease incidence (31.81%) and exhibited a higher disease reduction (52.56%), compared to the untreated control. Therefore, treatment with talc-based Streptomyces sp. isolate WAB2 is a sustainable solution for anthracnose disease management, and it facilitates eco-friendly crop protection practices against the disease in watermelon. RESEARCH HIGHLIGHTS: Isolated streptomycete strains from healthy watermelon plants and screened for its efficacy against the pathogen, Colletotrichum orbiculare WEC2. Streptomyces sp. isolate WAB2 showed significant antifungal activity against the pathogen. Bio-active compounds produced by Streptomyces sp. isolate WAB2 was identified by Gas Chromatography–Mass Spectrometry (GC–MS). Using scanning electron microscopy (SEM), the parasitic activity of Streptomyces sp. isolate WAB2 against the pathogen was detected. Developed a talc-based formulation of Streptomyces sp. isolate WAB2 and tested it as a seed treatment plus foliar spray, effectively reducing the disease incidence. Graphical abstract illustrating the isolation and characterisation of Streptomyces sp. isolate WAB2 for the management of anthracnose pathogen (Colletotrichum orbiculare WEC2) in Watermelon. Antagonistic potential of Streptomyces sp. isolate WAB2 against Colletotrichum orbiculare: [ABSTRACT FROM AUTHOR]

Published

2024

8. Streptomyces sp. from desert soil as a biofactory for antioxidants with radical scavenging and iron chelating potential.

Author

Shah, Imran, Uddin, Zia, Hussain, Maheer, Khalil, Atif Ali Khan, Amin, Arshia, Hanif, Faisal, Ali, Liaqat, Amirzada, Muhammad Imran, Shah, Tawaf Ali, Dawoud, Turki M., Bourhia, Mohammed, Li, Wen-Jun, and Sajjad, Wasim

Subjects

*ETHYLENEDIAMINE, *THIN layer chromatography, *IRON in the body, *EXTREME environments, *ANALYTICAL chemistry

Abstract

Iron homeostasis is vital for normal physiology, but in the majority of circumstances, like iron overload, this equilibrium is upset leading to free iron in the plasma. This condition with excess iron is known as hemochromatosis, which has been linked to many side effects, including cancer and liver cirrhosis. The current research aimed to investigate active molecules from Streptomyces sp. isolated from the extreme environment of Bahawalpur deserts. The strain was characterized using 16 S rRNA sequencing. Chemical analysis of the ethyl acetate cure extract revealed the presence of phenols, flavonoids, alkaloids, and tannins. Multiple ultraviolet (UV) active metabolites that were essential for the stated pharmacological activities were also demonstrated by thin layer chromatography (TLC) and high-performance liquid chromatography (HPLC). Additionally, Gas chromatography/mass spectrometry (GC-MS) analysis revealed the primary constituents of the extract to compose of phenol and ester compounds. The 2,2-diphenyl-1-picrylhydrazyl (DPPH) assay was used to assess the extract's antioxidant capacity, and the results showed a good half-maximal inhibitory concentration (IC50) value of 0.034 µg/mL in comparison to the positive control ascorbic acid's 0.12 µg/mL. In addition, iron chelation activity of extract showed significant chelation potential at 250 and 125 µg/mL, while 62.5 µg/mL showed only mild chelation of the ferrous ion using ethylene diamine tetra acetic acid (EDTA) as a positive control. Likewise, the extract's cytotoxicity was analyzed through 3-(4,5-Dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) assay using varying concentrations of the extract and showed 51% cytotoxicity at 350 µg/mL and 65% inhibition of cell growth at 700 µg/mL, respectively. The bioactive compounds from Streptomyces sp. demonstrated strong antioxidant and iron chelating potentials and can prolong the cell survival in extreme environment. [ABSTRACT FROM AUTHOR]

Published

2024

9. Identification of a polyphenol O-methyltransferase with broad substrate flexibility in Streptomyces albidoflavus J1074.

Author

Pérez-Valero, Álvaro, Magadán-Corpas, Patricia, Dulak, Kinga, Matera, Agata, Ye, Suhui, Huszcza, Ewa, Popłoński, Jarosław, Villar, Claudio J., and Lombó, Felipe

Subjects

*BIOCHEMICAL substrates, *COMPLEMENTATION (Genetics), *FLAVONOIDS, *CAFFEIC acid, *FLAVONES

Abstract

Flavonoids are a large and important group of phytochemicals with a great variety of bioactivities. The addition of methyl groups during biosynthesis of flavonoids and other polyphenols enhances their bioactivities and increases their stability. In a previous study of our research group, we detected a novel flavonoid O-methyltransferase activity in Streptomyces albidoflavus J1074, which led to the heterologous biosynthesis of homohesperetin from hesperetin in feeding cultures. In this study, we identify the O-methyltransferase responsible for the generation of this methylated flavonoid through the construction of a knockout mutant of the gene XNR_0417, which was selected after a blast analysis using the sequence of a caffeic acid 3′-O-methyltransferase from Zea mays against the genome of S. albidoflavus J1074. This mutant strain, S. albidoflavus ∆XNR_0417, was no longer able to produce homohesperetin after hesperetin feeding. Subsequently, we carried out a genetic complementation of the mutant strain in order to confirm that the enzyme encoded by XNR_0417 is responsible for the observed O-methyltransferase activity. This new strain, S. albidoflavus SP43-XNR_0417, was able to produce not only homohesperetin from hesperetin, but also different mono-, di-, tri- and tetra-methylated derivatives on other flavanones, flavones and stilbenes, revealing a broad substrate flexibility. Additionally, in vitro experiments were conducted using the purified enzyme on the substrates previously tested in vivo, demonstrating doubtless the capability of XNR_0417 to generate various methylated derivatives. [ABSTRACT FROM AUTHOR]

Published

2024

10. The involvement of multiple ABC transporters in daunorubicin efflux in Streptomyces coeruleorubidus.

Author

Dong, Jianxin, Ning, Jiali, Tian, Yu, Li, Han, Chen, Hua, and Guan, Wenjun

Subjects

*GENE clusters, *DAUNOMYCIN, *STREPTOMYCES, *LEUKEMIA, *EXTRUSION process, *ATP-binding cassette transporters

Abstract

Streptomyces genus produces a large number of antibiotics, which are always synthesized by specific biosynthetic gene clusters (BGCs). To resist autotoxicity, transporters encoded by genes located within BGC occasionally pump antibiotic along with transporter encoded by gene located outside BGC. Daunorubicin is an anthracycline antibiotic biosynthesized by Streptomyces species, playing a crucial role in the treatment of leukaemia. In existing studies, only one two‐component ATP‐binding cassette (ABC) transporter, encoded by drrA1‐drrB1 (abbreviated as drrAB1) and located within the daunorubicin BGC, has been proven to extrude daunorubicin. In this work, two other two‐component ABC transporters, encoded by drrAB2 and drrAB3 and located outside the cluster, were found to play the complementary role in daunorubicin efflux in S. coeruleorubidus. Disruption of three drrABs resulted in a 94% decrease in daunorubicin production. Furthermore, drrAB2 is regulated by the TetR family regulator DrrR1, responding to the intracellular accumulation of daunorubicin and suggesting its role in stress response and self‐resistance. Although the homologues of DrrAB1 are only found in three anthracycline BGCs, the homologues of DrrAB2 and DrrAB3 are spread in many Streptomyces strains which do not contain any known anthracycline BGC. This indicates that DrrAB2 and DrrAB3 may recognize and extrude a broader range of substrates besides daunorubicin, thus playing a more extensive role in cellular detoxification. [ABSTRACT FROM AUTHOR]

Published

2024

11. Antibacterial Compounds and Draft Genome Sequence of Streptomyces sp. PA5.6 Isolated from Deciduous Dipterocarp Forest Soils, University of Phayao, Thailand.

Author

Piyawan Amimanan, Wajeeorn Ouancharee, Noppadon Muangsue, Supakanya Lasom, and Nicha Charoensri

Subjects

*WHOLE genome sequencing, *ESCHERICHIA coli, *FOREST soils, *DECIDUOUS forests, *NUCLEOTIDE sequencing, *ACINETOBACTER baumannii

Abstract

Antibiotic resistance is a major problem in the control of infectious diseases. To overcome this obstacle, a common approach is to search for novel antimicrobial drugs from natural sources, especially microorganisms such as Streptomyces. Streptomyces has long been demonstrated to produce bioactive secondary metabolites with antimicrobial activities. The objectives of this research were to isolate and characterize Streptomyces strains from the deciduous dipterocarp forest soils in the University of Phayao, and to evaluate their metabolites for antibacterial activities. The results show that the morphological and physiological characteristics of PA5.6 are consistent with those of the genus Streptomyces. Furthermore, a comparative analysis of the whole genome sequence verified that PA5.6 represents a novel species within the genus Streptomyces. The genome sequence analysis of Streptomyces sp. PA5.6 revealed a total length of 9,146,340 bp, a G + C content of 71.1 %, and an N50 scaffold of 320,345 bp. The antiSMASH analysis revealed putative secondary metabolite Biosynthetic Gene Clusters (BGCs) involved in the biosynthesis of antimicrobial metabolites, including terpene, Type I PKS, NRPS and lassopeptide gene clusters. Functional prediction of these gene clusters indicates that they are involved in the biosynthesis of several antimicrobial-associated metabolites, such as albaflavenone, monensin and citrulassin D. Streptomyces sp. PA5.6 culture supernatant and its crude ethyl acetate extract exhibited antibacterial activity against several drug-resistant, bacterial pathogens, including S. aureus, E. faecalis, E. coli, P. aeruginosa, A. baumannii, MRSA, VREF, ESBL-E. coli and CRPA. The GC-MS analysis of the crude ethyl acetate extracts revealed benzeneacetic acid, benzeneacetic acid, 4-hydroxy and benzeneacetamide as major active compounds metabolites. In conclusion, Streptomyces sp. PA5.6 exhibited promising potential for producing bioactive compounds against bacterial pathogens. [ABSTRACT FROM AUTHOR]

Published

2024

12. Discovery of a novel methionine biosynthetic route via Ophospho-L-homoserine.

Author

Fumihito Hasebe, Kazuya Adachi, Chitose Maruyama, and Yoshimitsu Hamano

Subjects

*CARRIER proteins, *SECONDARY metabolism, *PROTEIN synthesis, *BLOCKCHAINS, *METABOLISM

Abstract

Methionine (Met), a sulfur-containing amino acid, is essential for the underlying biological processes in living organisms. In addition to its importance as a starting building block for peptide chain elongation in protein biosynthesis, Met is a direct precursor of S-adenosyl-L-methionine, an indispensable methyl donor molecule in primary and secondary metabolism. Streptomyces bacteria are well known to produce diverse secondary metabolites, but many strains lack canonical Met pathway genes for L-homocysteine, a direct precursor of Met in bacteria, plants, and archaea. Here, we report the identification of a novel gene (metM) responsible for the Met biosynthesis in Streptomyces strains and demonstrate the catalytic function of the gene product, MetM. We further identified the metO gene, a downstream gene of metM, and showed that it encodes a sulfur-carrier protein (SCP). In in vitro analysis, MetO was found to play an important role in a sulfur donor by forming a thiocarboxylated SCP. Together with MetO (thiocarboxylate), MetM directly converted O-phospho-L-homoserine to L-homocysteine. O-Phospho-L-homoserine is also known as an intermediate for threonine biosynthesis in bacteria and plants, and MetM shares sequence homology with threonine synthase. Our findings thus revealed that MetM seizes O-phospho-L-homoserine from the threonine biosynthetic pathway and uses it as an intermediate of the Met biosynthesis to generate the sulfur-containing amino acid. Importantly, this MetM/MetO pathway is highly conserved in Streptomyces bacteria and distributed in other bacteria and archaea. IMPORTANCE Methionine (Met) is a sulfur-containing proteinogenic amino acid. Moreover, Met is a direct precursor of S-adenosyl-L-methionine, an indispensable molecule for expanding the structural diversity of natural products. Because Met and its derivatives benefit humans, the knowledge of Met biosynthesis is important as a basis for improving their fermentation. Streptomyces bacteria are well known to produce diverse and valuable natural products, but many strains lack canonical Met pathway genes. Here, we identified a novel L-homocysteine synthase (MetM) in Streptomyces and demonstrated that it converts O-phospho-L-homoserine to L-homocysteine using a thiocarboxylated sulfur-carrier protein as a sulfur donor. Since the metM is distributed in other bacteria and archaea, our pioneering study contributes to understanding Met biosynthesis in these organisms. [ABSTRACT FROM AUTHOR]

Published

2024

13. Isolation, identification, and evaluation of the characteristics of Streptomyces sp. as the probiotic strains applied in aquaculture.

Author

Tam Pham Thi, Hien Nguyen Thi Thu, Huyen Vu Thi Bich, Mai Le Thi Tuyet, Hai Le Minh, Binh Ta Thi, Van Dao Thi Hong, Phuong Vo Hong, Thoa Vu Kim, Le Dinh Thi Thu, and Phuoc Man Hong

Subjects

*STREPTOMYCES, *PROBIOTICS, *AQUACULTURE, *SHRIMP diseases, *CATFISHES

Abstract

The present study was conducted to select Streptomyces strains that exhibited characteristics of probiotics for application in aquaculture. Streptomyces were isolated from soil and sediment samples collected from various habitats such as riverside, shrimp ponds, pangasius ponds, mangrove forests, or estuaries along the coast of Vietnam. Two strains of Streptomyces (AG12.2 and ND10.1) were selected due to (1) their potent antimicrobial activity against common pathogens that cause serious diseases in shrimp and pangasius such as E. ictaluri, A. hydophila, V. harveyi, V. parahaemolyticus, and (2) their superior ability to produce several extracellular enzymes that strongly hydrolyze organic compounds such as starch, CMC, and skimmed milk, compared to other strains. AG12.2 and ND10.1 can tolerate salinity from 0 ppt to 5 ppt and pH from 3 to 8; however, their growth is most vigorous at salt concentrations and pH between 0 ppt to 2 ppt, and 7.2 to 8, respectively. In vivo evaluation on L. vannamei in this study shows that shrimp that were fed with diets containing AG12.2 and ND10.1 had WG (%) increasing by 1.59 times and 1.61 times respectively, DGW (g/day) increasing by 1.64 times, and FCR decreasing by 1.30 times and 1.35 times respectively. The shrimp treated with AG12.2 and ND10.1 were then challenged with V. parahaemolyticus, resulting in a survival rate increase of 3.9 times and 3.71 times, respectively. Phylogenetic analysis revealed that strains AG12.2 and ND10.1 belong to Streptomyces kunmingensis and Streptomyces angustmyceticus, respectively. The findings of the present study led to the conclusion that Streptomyces kunmingensis AG12.2 and Streptomyces angustmyceticus ND10.1 are excellent candidates for producing beneficial probiotics for aquaculture. [ABSTRACT FROM AUTHOR]

Published

2024

14. The Chemistry of Angucyclines.

Author

Vysloužilová, Denisa and Kováč, Ondřej

Subjects

*NATURAL products, *POLYKETIDES, *CHEMISTS, *PHOTOOXIDATION, *STREPTOMYCES

Abstract

Angucyclines and angucyclinones represent a class of natural compounds that belong to the group of aromatic polyketides. They exhibit a wide array of biological properties, such as antimicrobial, antiviral, and cytotoxic. Their considerable therapeutic potential and diverse scaffolds have attracted many synthetic chemists to devise novel strategies to construct their intricate molecular architecture. Over 300 class members have been isolated from natural sources, mainly from bacterial strains of Streptomyces species. This review highlights recent advancements in their synthesis, such as oxidative cyclization, photooxidation, and metal‐catalyzed [4+2]‐cycloaddition, which has facilitated the efficient and practical total syntheses of various angucycline and angucyclinone natural products. [ABSTRACT FROM AUTHOR]

Published

2024

15. Central composite design for optimizing istamycin production by Streptomyces tenjimariensis.

Author

Gomaa, Fatma Alzahraa M., Selim, Heba Mohammed Refat M., Alshahrani, Mohammad Y., and Aboshanab, Khaled M.

Subjects

*RESPONSE surfaces (Statistics), *STATISTICAL models, *STREPTOMYCES, *ENVIRONMENTAL sciences, *ANTIBIOTICS

Abstract

Istamycins (ISMs) are 2-deoxyfortamine-containing aminoglycoside antibiotics (AGAs) produced by Streptomyces tenjimariensis ATCC 31603 with broad-spectrum bactericidal activities against most of the clinically relevant pathogens. Therefore, this study aimed to statistically optimize the environmental conditions affecting ISMs production using the central composite design (CCD). Both the effect of culture media composition and incubation time and agitation rate were studied as one factor at the time (OFAT). The results showed that both the aminoglycoside production medium and the protoplast regeneration medium gave the highest specific productivity. Results also showed that 6 days incubation time and 200 rpm agitation were optimum for their production. A CCD quadratic model of 17 runs was employed to test three key variables: initial pH, incubation temperature, and concentration of calcium carbonate. A significant statistical model was obtained including, an initial pH of 6.38, incubation temperature of 30 ˚C, and 5.3% CaCO3 concentration. This model was verified experimentally in the lab and resulted in a 31-fold increase as compared to the unoptimized conditions and a threefold increase to that generated by using the optimized culture media. To our knowledge, this is the first report about studying environmental conditions affecting ISM production as OFAT and through CCD design of the response surface methodology (RSM) employed for statistical optimization. In conclusion, the CCD design is an effective tool for optimizing ISMs at the shake flask level. However, the optimized conditions generated using the CCD model in this study should be scaled up in a fermenter for industrial production of ISMs by S. tenjimariensis ATCC 31603 considering the studied environmental conditions that significantly influence the production proces. [ABSTRACT FROM AUTHOR]

Published

2024

16. Natural products with γ-pyrone scaffold from Streptomyces.

Author

Magar, Rubin Thapa and Sohng, Jae Kyung

Subjects

*TRPV cation channels, *NATURAL products, *STREPTOMYCES, *CYTOTOXINS, *CHEMICAL structure, *POLYKETIDES

Abstract

The Streptomyces sp. is considered the vast reservoir of bioactive natural products belonging to different classes like polyketides, terpenoids, lanthipeptides, and non-ribosomal peptides to name a few. The ubiquitous distribution of the genus makes them capable of producing distinct compounds. Many of those compounds contain a unique γ-pyrone with various chemical structures and exhibit different bioactivities. One such class, nitrophenyl-γ-pyrone, constitutes different bioactive compounds isolated from Streptomyces sp. from different sources ranging from soil to marine environments. In addition, such compounds have antinematodal, cytotoxicity activities, and inhibition of adipogenesis. These compounds include aureothin (3), spectinabilin (7), and their derivatives. Moreover, there are other compounds like actinopyrones (11–16), benwamycins (22–23), and peucemycin and its derivatives (24–26) that also have antibacterial and anticancer activities. The other group classified as anthra-γ-pyrone has various bioactive natural products. For instance, tetrahydroanthra-γ-pyrone, shellmycin A-D (27–30) possess antibacterial as well as anticancer activities. In addition, the pluramycin family compounds belonging to anthra-γ-pyrone group also possess cytotoxic activity, for instance, kidamycin (31), rubiflavin, and their derivatives (33–37). Xanthones are another important group of natural products that also contain γ-pyrone ring producing different bioactivities. Albofungin (42) and its derivatives (43–46) belong to subgroup polycyclic tetrahydro xanthones that possess antibacterial, anticancer, and antibiofilm, antimacrofouling activities. Similarly, other compounds, belonging to this subgroup, exhibit different bioactivities like antifungal, antimalarial, and antibacterial activities and block transient receptor potential vanilloid 1 (TRPV1). These compounds include cervinomycins (48–55), citreamycins (56–57), sattahipmycin (59), and chrexanthomycins (60–63). This review gives succinct information on the γ-pyrone containing natural products isolated from Streptomyces sp. focusing on their structure and bioactivities. Key points: • The Streptomyces sp. is the producer of various bioactive natural products including the one with γ-pyrone ring. • These γ-pyrone compounds are structurally different and possess different bioactivities. • The Streptomyces has the potential to produce such compounds and the reservoir of these compounds is expected to increase in the future. [ABSTRACT FROM AUTHOR]

Published

2024

17. Isolation and characterization of plant‐pathogenic Streptomyces species associated with potato common scab disease in Türkiye.

Author

Uysal, Nida, Bozkurt, Adem, and Elçi, Eminur

Subjects

*TUBERS, *STREPTOMYCES, *SPECIES distribution, *SEQUENCE analysis, *PHYLOGENY, *POTATOES

Abstract

Potato common scab (PCS), a significant potato disease, negatively impacts tuber quality. The present study was conducted to isolate and characterize pathogenic Streptomyces species associated with PCS disease in Türkiye based on their morphological, physiological and molecular characteristics. Field‐grown potatoes that exhibited scab lesions were collected from four provinces in 2020–2021, and 200 bacterial isolates were obtained from netted, superficial and deep‐pitted common scab lesions. Pathogenicity assays, including in vitro tuber slice and in planta radish seedling bioassays, identified 150 pathogenic isolates. Morphological and physiological characterization of 92 selected isolates revealed several Streptomyces species that exhibited diverse mycelium colours, sporulation patterns and pigmentation. Molecular analysis using 16S rRNA sequencing, species‐specific primers, PCR‐RFLP of the 16S‐23S (ITS) region with Hpy99I restriction enzyme, and multilocus sequence analysis (MLSA) based on atpD, recA, rpoB and trpB genes revealed that S. scabiei was the dominant species, followed by S. europaeiscabiei, S. caniscabiei, S. bottropensis, S. stelliscabiei and S. turgidiscabies. PCR analysis revealed the presence of the thaxtomin synthetase genes (txtAB) in all tested samples, while the necrogenic protein (nec1) and tomatinase (tomA)‐encoding genes were absent from three and two isolates, respectively. Phylogenetic analysis of 32 representative isolates conducted with sequences from 16S rRNA, species‐specific PCR and MLSA confirmed their morphological identification and clustered them with reference strains. This study contributes to the understanding of distribution of Streptomyces species associated with PCS, and to our knowledge, is the first molecular confirmation of S. caniscabiei and S. turgidiscabies causing potato scab in Türkiye. [ABSTRACT FROM AUTHOR]

Published

2024

18. Deciphering domain structures of Aspergillus and Streptomyces GH3-β-Glucosidases: a screening system for enzyme engineering and biotechnological applications.

Author

Sidar, Andika, Voshol, Gerben P., Arentshorst, Mark, Ram, Arthur F.J., Vijgenboom, Erik, and Punt, Peter J.

Subjects

*FILAMENTOUS bacteria, *INDUSTRIAL enzymology, *ASPERGILLUS niger, *BIOTECHNOLOGY, *GLUCOSIDASES, *CATALYTIC domains

Abstract

The glycoside hydrolase family 3 (GH3) β-glucosidases from filamentous fungi are crucial industrial enzymes facilitating the complete degradation of lignocellulose, by converting cello-oligosaccharides and cellobiose into glucose. Understanding the diverse domain organization is essential for elucidating their biological roles and potential biotechnological applications. This research delves into the variability of domain organization within GH3 β-glucosidases. Two distinct configurations were identified in fungal GH3 β-glucosidases, one comprising solely the GH3 catalytic domain, and another incorporating the GH3 domain with a C-terminal fibronectin type III (Fn3) domain. Notably, Streptomyces filamentous bacteria showcased a separate clade of GH3 proteins linking the GH3 domain to a carbohydrate binding module from family 2 (CBM2). As a first step to be able to explore the role of accessory domains in β-glucosidase activity, a screening system utilizing the well-characterised Aspergillus niger β-glucosidase gene (bglA) in bglA deletion mutant host was developed. Based on this screening system, reintroducing the native GH3-Fn3 gene successfully expressed the gene allowing detection of the protein using different enzymatic assays. Further investigation into the role of the accessory domains in GH3 family proteins, including those from Streptomyces, will be required to design improved chimeric β-glucosidases enzymes for industrial application. [ABSTRACT FROM AUTHOR]

Published

2024

19. A new synthetic biology system for investigating the biosynthesis of antibiotics and other secondary metabolites in streptomycetes.

Author

Javorova, Rachel, Rezuchova, Bronislava, Feckova, Lubomira, Novakova, Renata, Csolleiova, Dominika, Kopacova, Maria, Patoprsty, Vladimir, Opaterny, Filip, Sevcikova, Beatrica, and Kormanec, Jan

Subjects

*SYSTEMS biology, *MOLECULAR cloning, *GENE clusters, *CHROMOSOMES, *METABOLITES, *SYNTHETIC biology

Abstract

We have created a novel synthetic biology expression system allowing easy refactoring of biosynthetic gene clusters (BGCs) as monocistronic transcriptional units. The system is based on a set of plasmids containing a strong kasOp* promoter, RBS and terminators. It allows the cloning of biosynthetic genes into transcriptional units kasOp *-gene(s)-terminator flanked by several rare restriction cloning sites that can be sequentially combined into the artificial BGC in three compatible Streptomyces integration vectors. They allow a simultaneous integration of these BGCs at three different attB sites in the Streptomyces chromosome. The system was validated with biosynthetic genes from two known BGCs for aromatic polyketides landomycin and mithramycin. • A new synthetic biology-based system for investigating antibiotic biosynthesis. • Efficient rabelomycin production using the initial landomycin biosynthetic genes. • Efficient 4-DMPC production using the initial mithramycin biosynthetic genes. [ABSTRACT FROM AUTHOR]

Published

2024

20. Analysis of secondary metabolites and morphology in Streptomyces rimosus microparticle-enhanced cultivation (MPEC) at various initial organic nitrogen concentrations.

Author

Ścigaczewska, Anna, Boruta, Tomasz, Grzesiak, Weronika, and Bizukojć, Marcin

Subjects

*YEAST extract, *METABOLITES, *TALC, *OXYTETRACYCLINE, *STREPTOMYCES

Abstract

The influence of talc microparticles on metabolism and morphology of S. rimosus at various initial organic nitrogen concentrations was investigated. The shake flask cultivations were conducted in the media with yeast extract (nitrogen source) concentration equal to 1 g YE L− 1 and 20 g YE L− 1. Two talc microparticle concentrations of 5 g TALC L− 1 and 10 g TALC L− 1 were tested in microparticle-enhanced cultivation (MPEC) runs. A high nitrogen concentration of 20 g YE L− 1 promoted the development of small agglomerates (pellets) of projected area lower than 105 µm2 and dispersed pseudohyphae. A low nitrogen concentration of 1 g YE L− 1 led to the limitation of S. rimosus growth and, in consequence, the development of the smaller number of large pseudohyphal agglomerates (pellets) of projected area higher than 105 µm2 compared to the culture containing a high amount of nitrogen source. In both cases talc microparticles were embedded into pellets and caused the decrease in their sizes. The lower amount of talc (5 g TALC L− 1) usually caused the weaker effect on S. rimosus morphology and metabolite production than the higher one. This correlation between the microparticles effect on morphology and metabolism of S. rimosus was especially noticeable in the biosynthesis of oxytetracycline, 2-acetyl-2-dicarboxamide oxytetracycline (ADOTC) and spinoxazine A. Compared to the control run, in MPEC their levels increased 4-fold, 5-fold and 1.6-fold respectively. The addition of talc also improved the production of 2-methylthio-cis-zeatin, lorneic acid J and milbemycin A3. [ABSTRACT FROM AUTHOR]

Published

2024

21. Streptomyces avermitilis MICNEMA2022: a new biorational strain for producing abamectin as an integrated nematode management agent.

Author

Radwan, Wafaa H., Abdelhafez, Ahmed A. M., Mahgoub, Ahmed E., and Zayed, Mona S.

Subjects

*ABAMECTIN, *SOUTHERN root-knot nematode, *RF values (Chromatography), *ROOT-knot, *STREPTOMYCES

Abstract

Background: Abamectin (ABA) is considered a powerful insecticidal and anthelmintic agent. It is an intracellular product of Streptomyces avermitilis; is synthesized through complicated pathways and can then be extracted from mycelial by methanol extraction. ABA serves as a biological control substance against the root-knot nematode Meloidogyne incognita. This investigation is intended to reach a new strain of S. avermitilis capable of producing ABA effectively. Results: Among the sixty actinobacterial isolates, Streptomyces St.53 isolate was chosen for its superior nematicidal effectiveness. The mycelial-methanol extract of isolate St.53 exhibited a maximum in vitro mortality of 100% in one day. In the greenhouse experiment, the mycelial-methanol extract demonstrated, for the second-stage juveniles (J2s), 75.69% nematode reduction and 0.84 reproduction rate (Rr) while for the second-stage juveniles (J2s), the culture suspension demonstrated 75.38% nematode reduction and 0.80 reproduction rate (Rr). Molecular identification for St.53 was performed using 16 S rRNA gene analysis and recorded in NCBI Genbank as S. avermitilis MICNEMA2022 with accession number (OP108264.1). LC-MS was utilized to detect and identify abamectin in extracts while HPLC analysis was carried out for quantitative determination. Both abamectin B1a and abamectin B1b were produced and detected at retention times of 4.572 and 3.890 min respectively. Conclusion: Streptomyces avermitilis MICNEMA2022 proved to be an effective source for producing abamectin as a biorational agent for integrated nematode management. [ABSTRACT FROM AUTHOR]

Published

2024

22. Hirocidins, Cytotoxic Metabolites from Streptomyces hiroshimensis, Induce Mitochondrion‐Mediated Apoptosis.

Author

Han, Esther J., Jeong, Myungeun, Lee, Seoung Rak, Sorensen, Erik J., and Seyedsayamdost, Mohammad R.

Subjects

*STREPTOMYCES, *WHOLE genome sequencing, *DRUG discovery, *METABOLITES, *SMALL molecules, *APOPTOSIS, *CANCER cells

Abstract

Recent advances in whole genome sequencing have revealed an immense microbial potential for the production of therapeutic small molecules, even from well‐known producers. To access this potential, we subjected prominent antimicrobial producers to alternative antiproliferative assays using persistent cancer cell lines. Described herein is our discovery of hirocidins, novel secondary metabolites from Streptomyces hiroshimensis with antiproliferative activities against colon and persistent breast cancer cells. Hirocidin A is an unusual nine‐membered carbocyclic maleimide and hirocidins B and C are relatives with an unprecedented, bridged azamacrocyclic backbone. Mode of action studies show that hirocidins trigger mitochondrion‐dependent apoptosis by inducing expression of the key apoptotic effector caspase‐9. The discovery of new cytotoxins contributes to scaffold diversification in anticancer drug discovery and the reported modes of action and concise total synthetic route for variant A set the stage for unraveling specific targets and biochemical interactions of the hirocidins. [ABSTRACT FROM AUTHOR]

Published

2024

23. Heterologous expression of lasso peptides with apparent participation in the morphological development in Streptomyces.

Author

Reyna-Campos, Alma Ofelia, Ruiz-Villafan, Beatriz, Macías-Rubalcava, Martha Lydia, Langley, Elizabeth, Rodríguez-Sanoja, Romina, and Sánchez, Sergio

Subjects

*METABOLITES, *PHENOTYPIC plasticity, *GENE clusters, *PEPTIDES, *STREPTOMYCES

Abstract

Lasso peptides, ribosomally synthesized and post-translationally modified peptides, are primarily produced by bacteria and some archaea. Streptomyces lasso peptides have been known for their antimicrobial, anticancer, and antiviral properties. However, understanding their role in the morphology and production of secondary metabolites remains limited. We identified a previously unknown lasso peptide gene cluster in the genome of Streptomyces sp. L06. This gene cluster (LASS) produces two distinct lasso peptides, morphosin-1 and − 2. Notably, morphosin-2 is a member of a new subfamily of lasso peptides, with BGCs exhibiting a similar structure. When LASS was expressed in different Streptomyces hosts, it led to exciting phenotypic changes, including the absence of spores and damage in aerial mycelium development. In one of the hosts, LASS even triggered antibiotic formation. These findings open up a world of possibilities, suggesting the potential role of morphosins in shaping Streptomyces' morphological and biochemical development. [ABSTRACT FROM AUTHOR]

Published

2024

24. Streptomyces pratensis S10 Inhibits the Spread of Fusarium graminearum Invasive Hyphae and Toxisome Formation in Wheat Plants.

Author

Lifang Hu, Jing Chen, Ruimin Jia, Yan Sun, Xiaomin Dong, Shang Cao, Xihui Shen, and Yang Wang

Subjects

*GENE expression, *WHEAT, *STREPTOMYCES, *CULTIVARS, *PHLOEM

Abstract

Fusarium head blight (FHB) of wheat, mainly caused by Fusarium graminearum, leads to severe economic losses worldwide. Effective management measures for controlling FHB are not available due to a lack of resistant cultivars. Currently, the utilization of biological control is a promising approach that can be used to help manage FHB. Previous studies have confirmed that Streptomyces pratensis S10 harbors excellent inhibitory effects on F. graminearum. However, there is no information regarding whether invasive hyphae of F. graminearum are inhibited by S10. Thus, we investigated the effects of S10 on F. graminearum strain PH-1 hypha extension, toxisome formation, and TRI5 gene expression on wheat plants via microscopic observation. The results showed that S10 effectively inhibited the spread of F. graminearum hyphae along the rachis, restricting the infection of neighboring florets via the phloem. In the presence of S10, the hyphal growth is impeded by the formation of dense cell wall thickenings in the rachis internode surrounding the F. graminearum infection site, avoiding cell plasmolysis and collapse. We further demonstrated that S10 largely prevented cell-to-cell invasion of fungal hyphae inside wheat coleoptiles using a constitutively green fluorescence protein-expressing F. graminearum strain, PH-1. Importantly, S. pratensis S10 inhibited toxisome formation and TRI5 gene expression in wheat plants during infection. Collectively, these findings indicate that S. pratensis S10 prevents the spread of F. graminearum invasive hyphae via the rachis. [ABSTRACT FROM AUTHOR]

Published

2024

25. Antibacterial compounds derived from marine Streptomyces aureofaciens A3 through in-silico molecular docking.

Author

Srikandace, Yoice, Syani, Ira Rhabbiyatun, Wahhaab, Aisha, Kamarisima, Putri, Sastia P., and Aditiawati, Pingkan

Abstract

Streptomyces aureofaciens widely produces the antibiotic tetracycline and many other compounds during fermentation. The compounds have yet to be known for their antibacterial potential. This work aims to determine new antibiotics or other possible antibacterial compounds produced by marine S.aureofaceiens A3 through an in silico molecular docking method. The ethyl acetate (EA) extracts from fermented marine S. aureofaciens A3 in ISP4 medium enriched with seawater components showed strong antibacterial activity. The antibacterial activity of EA extracts during 6-12 days of fermentation was carried out by the Kirby-Bauer method and the compounds of EA extracts were analyzed by GC/MS. Compounds identified by GC/MS were ligands for an in silico molecular docking study against four target proteins (DNA gyrase, topoisomerase IV, PBP 1a, and DHFR) of pathogenic bacteria. The drug-likeness of selected chemicals as antibacterial agents was assessed using Lipinski's Rule of Five. The results showed the prospective compounds as a narrow-spectrum antibacterial, including 3,5-di-tert-Butyl-4-hydroxyphenylpropionic acid against PBP 1a and Benzenepropanoic acid, and 3,5-bis (1,1-dimethyl ethyl)-4-hydroxy-, methyl esters against DHFR. Substances with broad-spectrum antibacterial activity, such as 3-Acetylphenanthrene and 3-(p-Ethoxyphenyl)-5-(O-tolyloxymethyl)-2-oxazolidone, against multitarget DNA gyrase B and DHFR, 7,9-Di-tert-butyl-1-oxaspiro (4,5) Deca-6,9-diene-2,8-dione against PBP1a and DHFR, and isobenzofuro [5,6-b] benzofuran-8-carboxylic acid, 1,3-dihydro-7,10-dimethoxy-9-methyl-1-oxo-, methyl ester against DNA gyrase B, PBP 1a, and DHFR. On the 12th day of fermentation, two compounds were identified: isobenzofuro[5,6-b] benzofuran-8-carboxylic acid, 1,3-dihydro-7,10-dimethoxy-9-methyl-1-oxo-, methyl ester, and 3-(p-Ethoxyphenyl)-5-(O-tolyl oxy methyl)-2-oxazolidone. This is the first report that these two compounds, known as potential drugs like antibiotics through in silico molecular docking, were first produced by Streptomyces species. [ABSTRACT FROM AUTHOR]

Published

2024

26. Harnessing Plant Growth–Promoting and Wilt‐Controlling Biopotential of a Consortium of Actinomycetes and Mycorrhizae in Pigeon Pea.

Author

Dave, Anand, Ingle, Sanjay, Perveen, Kahkashan, Bukhari, Najat A., Sayyed, Riyaz, and Mastinu, Andrea

Subjects

*PLANT growth, *GRAIN yields, *DISEASE management, *POTTED plants, *REVENUE management, *MICROBIAL inoculants

Abstract

Fusarium‐induced wilt significantly affects the cultivation and yield of pigeon peas. This warrants sustainable disease management while promoting plant growth. The present study investigated the biopotential of coinoculation of Streptomyces pseudogriseolus S‐9 and Rhizophagus irregularis for plant growth promotion and mitigation of the impact of Fusarium wilt on pigeon pea over three seasons at pot and field levels. Pigeon pea plants were subjected to Fusarium wilt stress and treated with different inoculation strategies, including single and combined applications of S. pseudogriseolus S‐9 and R. irregularis. Plant growth parameters and yields were assessed to evaluate the efficacy of the coinoculation. In the pot experiment, T‐6 treatment resulted in the longest root (62.56 ± 0.01 cm) and shoot (70.24 ± 0.01 cm) lengths compared to the application of commercial biofungicide T‐8 (Trichoderma). This treatment also significantly influenced the yield of potted plants. It resulted in the highest fresh root weight (62.27 ± 0.01 g), fresh shoot weight (70.24 ± 0.02 g), maximum root (55.25 ± 0.01 g) and shoot dry weights (52.25 ± 0.01 g). In the field experiment, pigeon pea plants treated with the bioinoculant also demonstrated a substantial increase (р ≤ 0.05) in total grain yield, the weight of 100 grains, and the number of filled grains compared to the control group in all experimental seasons. In vitro, antagonism assay of compatibility of mycorrhizae and bacteria showed good activity using powder formulation. Thus, the consortium application inspired the broad application of Streptomyces and Trichoderma as effective bioinoculants for wilt management and yield improvement in pigeon peas. [ABSTRACT FROM AUTHOR]

Published

2024

27. Genome Mining for Diazo-Synthesis-Related Genes in Streptomyces sp. CS057 Unveiled the Cryptic Biosynthetic Gene Cluster crx for the Novel 3,4-AHBA-Derived Compound Crexazone 2.

Author

Prado-Alonso, Laura, Ye, Suhui, Pérez-Victoria, Ignacio, Montero, Ignacio, Riesco, Pedro, Ortiz-López, Francisco Javier, Martín, Jesús, Olano, Carlos, Reyes, Fernando, and Méndez, Carmen

Subjects

*LEAF-cutting ants, *REGULATOR genes, *GENE clusters, *GROUP formation, *STREPTOMYCES

Abstract

Natural products play a crucial role in drug development, addressing the escalating microbial resistance to antibiotics and the treatment of emerging diseases. Progress in genome sequencing techniques, coupled with the development of bioinformatics tools and the exploration of uncharted habitats, has highlighted the biosynthetic potential of actinomycetes. By in silico screening for diazo-related gene genomes from twelve Streptomyces strains isolated from Attini leaf-cutting ants, the new crx biosynthetic gene cluster (BGC) was identified in Streptomyces sp. CS057. This cluster, highly conserved in several Streptomyces strains, contains genes related to diazo group formation and genes for the biosynthesis of 3,4-AHBA. By overexpressing the LuxR-like regulatory gene crxR1, we were able to activate the crx cluster, which encodes the biosynthesis of three 3,4-AHBA-derived compounds that we named crexazones (CRXs). The chemical structure of crexazones (CRXs) was determined by LC-DAD-HRMS-based dereplication and NMR spectroscopic analyses and was found to correspond to two known compounds, 3-acetamido-4-hydroxybenzoic acid (CRX1) and the phenoxazinone texazone (CRX3), and a novel 3,4-AHBA-containing compound herein designated as CRX2. Experimental proof linking the crx BGC to their encoded compounds was achieved by generating mutants in selected crx genes. [ABSTRACT FROM AUTHOR]

Published

2024

28. Rational construction of genome-minimized Streptomyces host for the expression of secondary metabolite gene clusters.

Author

Hui Li, Sheng Gao, Sanyuan Shi, Xiaomin Zha, Haoyu Ye, and Yunzi Luo

Subjects

*GENE expression, *GENOME size, *SYNTHETIC products, *SYNTHETIC biology, *CRISPRS

Abstract

Streptomyces offer a wealth of naturally occurring compounds with diverse structures, many of which possess significant pharmaceutical values. However, new product exploration and increased yield of specific compounds in Streptomyces have been technically challenging due to their slow growth rate, complex culture conditions and intricate genetic backgrounds. In this study, we screened dozens of Streptomyces strains inhabiting in a plant rhizosphere for fast-growing candidates, and further employed CRISPR/Cas-based engineering techniques for stepwise refinement of a particular strain, Streptomyces sp. A-14 that harbors a 7.47 Mb genome. After strategic removal of nonessential genomic regions and most gene clusters, we reduced its genome size to 6.13 Mb, while preserving its growth rate to the greatest extent. We further demonstrated that cleaner metabolic background of this engineered strain was well suited for the expression and characterization of heterologous gene clusters, including the biosynthetic pathways of actinorhodin and polycyclic tetramate macrolactams. Moreover, this streamlined genome is anticipated to facilitate directing the metabolic flux towards the production of desired compounds and increasing their yields. [ABSTRACT FROM AUTHOR]

Published

2024

29. Analyzing and engineering of the biosynthetic pathway of mollemycin A for enhancing its production.

Author

Shixue Jin, Huixue Chen, Jun Zhang, Zhi Lin, Xudong Qu, Xinying Jia, and Chun Lei

Subjects

*SUSTAINABILITY, *GENE clusters, *PLASMODIUM, *STREPTOMYCES, *FERMENTATION

Abstract

Mollemycin A (MOMA) is a unique glyco-hexadepsipeptide-polyketide that was isolated from a Streptomyces sp. derived from the Australian marine environment. MOMA exhibits remarkable inhibitory activity against both drug-sensitive and multidrug-resistant malaria parasites. Optimizing MOMA through structural modifications or product enhancements is necessary for the development of effective analogues. However, modifying MOMA using chemical approaches is challenging, and the production titer of MOMA in the wild-type strain is low. This study identified and characterized the biosynthetic gene cluster of MOMA for the first time, proposed its complex biosynthetic pathway, and achieved an effective two-pronged enhancement of MOMA production. The fermentation medium was optimized to increase the yield of MOMA from 0.9 mg L−1 to 1.3 mg L− 1, a 44% boost. Additionally, a synergistic mutant strain was developed by deleting the momB3 gene and overexpressing momB2, resulting in a 2.6-fold increase from 1.3 mg L− 1 to 3.4 mg L− 1 . These findings pave the way for investigating the biosynthetic mechanism of MOMA, creating opportunities to produce a wide range of MOMA analogues, and developing an efficient strain for the sustainable and economical production of MOMA and its analogues. [ABSTRACT FROM AUTHOR]

Published

2024

30. Unleashing the potential: type I CRISPR-Cas systems in actinomycetes for genome editing.

Author

Shuliu Wang, Xiaoqian Zeng, Yue Jiang, Weishan Wang, Linquan Bai, Yinhua Lu, Lixin Zhang, and Gao-Yi Tan

Subjects

*GENOME editing, *ACTINOBACTERIA, *NATURAL products, *STREPTOMYCES, *ARCHAEBACTERIA, *CRISPRS

Abstract

Type I CRISPR-Cas systems are widely distributed, found in over 40% of bacteria and 80% of archaea. Among genome-sequenced actinomycetes (particularly Streptomyces spp.), 45.54% possess type I CRISPR-Cas systems. In comparison to widely used CRISPR systems like Cas9 or Cas12a, these endogenous CRISPRCas systems have significant advantages, including better compatibility, wide distribution, and ease of operation (since no exogenous Cas gene delivery is needed). Furthermore, type I CRISPR-Cas systems can simultaneously edit and regulate genes by adjusting the crRNA spacer length. Meanwhile, most actinomycetes are recalcitrant to genetic manipulation, hindering the discovery and engineering of natural products (NPs). The endogenous type I CRISPR-Cas systems in actinomycetes may offer a promising alternative to overcome these barriers. This review summarizes the challenges and recent advances in CRISPR-based genome engineering technologies for actinomycetes. It also presents and discusses how to establish and develop genome editing tools based on type I CRISPR-Cas systems in actinomycetes, with the aim of their future application in gene editing and the discovery of NPs in actinomycetes. [ABSTRACT FROM AUTHOR]

Published

2024

31. Biotransformation of monoterpenes using Streptomyces strains from the rhizosphere of Inga edulis Martius from in an Amazonian urban forest fragment.

Author

Sevalho, Elison de Souza, de Souza Rodrigues, Rafael, Queiroz Lima de Souza, Antonia, and Duarte Leão de Souza, Afonso

Subjects

*FOOD additives, *GAS chromatography/Mass spectrometry (GC-MS), *ACTINOBACTERIA, *STREPTOMYCES, *MONOTERPENES

Abstract

To investigate the biocatalytic potential of Amazonian actinomycetes for monoterpenes biotransformation. To carry out the present study, eleven actinomycetes of the genus Streptomyces isolated from inga-cipó (Inga edulis Mart.) rhizospheres were tested for their ability to bioconvert the substrates R-(+)-limonene, S-(-)-limonene, 1S-(-)-α-pinene, and (-)–β–pinene as sole carbon and energy source. According to gas chromatography-mass spectrometry analysis, three strains, LabMicra B270, LaBMicrA B310, and LaBMicrA B314, were able to biotransform 1S-(-)-α-pinene after 96 h of growth. However, Streptomyces LaBMicrA B270 was the most promising since it converted after only 72 h all the 1S-(-)-α-pinene mainly into cis-verbenol (74.9±1.24%) and verbenone (18.2±1.20%), compounds that have important biological activities and great industrial interest as additives in foods and cosmetics. These findings can stimulate the development of natural aromas using naturally abundant monoterpenes, ratify the potential of microorganisms from almost unexplored niches such as the Amazonian rhizosphere, and reinforce the importance of preserving those niches. [ABSTRACT FROM AUTHOR]

Published

2024

32. Characterization of the equine placental microbial population during nocardioform placentitis.

Author

van Heule, Machteld, El-Sheikh Ali, Hossam, Monteiro, Hugo Fernando, Scoggin, Kirsten, Fedorka, Carleigh, Weimer, Bart C., Ball, Barry, Daels, Peter, and Dini, Pouya

Subjects

*GRAM-positive bacteria, *CHORIOALLANTOIS, *PLACENTA, *ENTEROCOCCUS, *STREPTOMYCES, *MICROBIAL diversity

Abstract

Nocardioform placentitis is a poorly understood disease of equine late gestation. The presence of nocardioform, filamentous branching gram-positive bacteria, has been linked to the disease, with Crossiella equi , Amycolatopsis spp., and Streptomyces spp. being the most frequently identified bacteria. However, these bacteria are not found in all clinical cases in addition to being isolated from healthy, normal postpartum placentas. To better understand this form of placentitis, we analyzed the microbial composition in the equine placenta (chorioallantois) of both healthy postpartum (control; n = 11) and nocardioform-affected samples (n = 22) using 16S rDNA sequencing. We found a lower Shannon index in nocardioform samples, a higher Chao1 index in nocardioform samples, and a difference in beta diversity between control and nocardioform samples (p < 0.05), suggesting the presence of dysbiosis during the disease. In the majority of the NP samples (77 %), one of the following genera— Amycolatopsis , Crossiella , Lentzea , an unidentified member of the Pseudonocardiaceae family, Mycobacterium, or Enterococcus —represented over 70 % of the relative abundance. Overall, the data suggest that a broader spectrum of potential opportunistic pathogens could be involved in nocardioform placentitis, extending beyond the traditionally recognized bacteria, resulting in a similar histomorphological profile. • Non-nocardioform opportunistic pathogens may be associated with placentitis. • Nocardioform placentitis is associated with dysbiotic changes. • Nocardioform placentitis exhibits a unique microbial diversity distinct from control samples. [ABSTRACT FROM AUTHOR]

Published

2024

33. Initial pH determines the morphological characteristics and secondary metabolite production in Aspergillus terreus and Streptomyces rimosus cocultures.

Author

Boruta, Tomasz, Foryś, Martyna, Pawlikowska, Weronika, Englart, Grzegorz, and Bizukojć, Marcin

Subjects

*AXENIC cultures, *ASPERGILLUS terreus, *METABOLITES, *STREPTOMYCES, *PH effect

Abstract

The influence of the initial pH on the morphology and secondary metabolite production in cocultures and axenic cultures of Aspergillus terreus and Streptomyces rimosus was investigated. The detected secondary metabolites (6 of bacterial and 4 of fungal origin) were not found in the cultures initiated at pH values less than or equal to 4.0. The highest mean levels of oxytetracycline were recorded in S. rimosus axenic culture at pH 5.0. Initiating the axenic culture at pH 5.9 led to visibly lower product levels, yet the presence of A. terreus reduced the negative effect of non-optimal pH and led to higher oxytetracycline titer than in the corresponding S. rimosus axenic culture. The cocultivation initiated at pH 5.0 or 5.9 triggered the formation of oxidized rimocidin. The products of A. terreus were absent in the cocultures. At pH 4.0, the striking morphological differences between the coculture and the axenic cultures were recorded. [ABSTRACT FROM AUTHOR]

Published

2024

34. Diversity and Bioactivity of Endophytic Actinobacteria Associated with the Roots of Artemisia herba-alba Asso from Algeria.

Author

Djemouai, Nadjette, Meklat, Atika, Youcef, Khadidja Oulad Hadj, Nacer, Asma, Saadi, Sid Ahmed, and Verheecke-Vaessen, Carol

Subjects

*GRAM-positive bacteria, *ARID regions, *NITROGEN fixation, *ATMOSPHERIC nitrogen, *STREPTOMYCES, *ACTINOBACTERIA

Abstract

The isolation of endophytic actinobacteria from the roots of wild populations of Artemisia herba-alba Asso, a medicinal plant collected from the arid lands of Algeria, is reported for the first time. Forty-five actinobacterial isolates were identified by molecular analysis and in vitro evaluated for antimicrobial activity and plant growth-promoting (PGP) abilities (1-Aminocyclopropane-1-carboxylic acid (ACC) deaminase activity, nitrogen fixation, phosphate and potassium solubilization, ammonia, and siderophores production). The phylogenetic relationships based on 16S rRNA gene sequences show that the genus Nocardioides (n = 23) was dominant in the sampled localities. The remaining actinobacterial isolates were identified as Promicromonospora (n = 11), Streptomyces (n = 6), Micromonopora (n = 3), and Saccharothrix (n = 2). Only six (13.33%) strains (five Streptomyces and one Saccharothrix species) were antagonistic in vitro against at least one or more indicator microorganisms. The antimicrobial activity of actinobacterial strains targeted mainly Gram-positive bacteria. The results demonstrate that more than 73% of the isolated strains had ACC deaminase activity, could fix atmospheric nitrogen and were producers of ammonia and siderophores. However, only one (2.22%) strain named Saccharothrix sp. BT79 could solubilize phosphorus and potassium. Overall, many strains exhibited a broad spectrum of PGP abilities. Thus, A. herba-alba provides a source of endophytic actinobacteria that should be explored for their potential biological activities. [ABSTRACT FROM AUTHOR]

Published

2024

35. Functional connexion of bacterioferritin in antibiotic production and morphological differentiation in Streptomyces coelicolor.

Author

García-Martín, Javier, García-Abad, Laura, Santamaría, Ramón I., and Díaz, Margarita

Subjects

*STREPTOMYCES coelicolor, *RIBOSOMAL proteins, *IRON proteins, *REACTIVE oxygen species, *METABOLIC regulation, *FERRITIN

Abstract

Background: Several two-component systems of Streptomyces coelicolor, a model organism used for studying antibiotic production in Streptomyces, affect the expression of the bfr (SCO2113) gene that encodes a bacterioferritin, a protein involved in iron storage. In this work, we have studied the effect of the deletion mutant ∆bfr in S. coelicolor. Results: The ∆bfr mutant exhibits a delay in morphological differentiation and produces a lesser amount of the two pigmented antibiotics (actinorhodin and undecylprodigiosin) compared to the wild type on complex media. The effect of iron in minimal medium was tested in the wild type and ∆bfr mutant. Consequently, we also observed different levels of production of the two pigmented antibiotics between the two strains, depending on the iron concentration and the medium (solid or liquid) used. Contrary to expectations, no differences in intracellular iron concentration were detected between the wild type and ∆bfr mutant. However, a higher level of reactive oxygen species in the ∆bfr mutant and a higher tolerance to oxidative stress were observed. Proteomic analysis showed no variation in iron response proteins, but there was a lower abundance of proteins related to actinorhodin and ribosomal proteins, as well as others related to secondary metabolite production and differentiation. Additionally, a higher abundance of proteins related to various types of stress, such as respiration and hypoxia among others, was also revealed. Data are available via ProteomeXchange with identifier PXD050869. Conclusion: This bacterioferritin in S. coelicolor (Bfr) is a new element in the complex regulation of secondary metabolism in S. coelicolor and, additionally, iron acts as a signal to modulate the biosynthesis of active molecules. Our model proposes an interaction between Bfr and iron-containing regulatory proteins. Thus, identifying these interactions would provide new information for improving antibiotic production in Streptomyces. [ABSTRACT FROM AUTHOR]

Published

2024

36. Proteolysis-resistant extracellular uricase from the sponge-derived <italic>Streptomyces rochei</italic>.

Author

Arslan Ece, Merve, Kocadağ Kocazorbaz, Ebru, and Hameş, Elif Esin

Subjects

*ION exchange chromatography, *MARINE microorganisms, *FILAMENTOUS fungi, *MOLECULAR weights, *STREPTOMYCES, *ACTINOBACTERIA

Abstract

AbstractThis study aimed to identify proteolysis-resistant extracellular uricase by screening three hundred marine microorganisms, including bacteria, actinobacteria and filamentous fungi. The isolate, demonstrating resistance to proteolysis and producing extracellular uricase with relatively high activity was identified as Streptomyces rochei 6SM85. The enzyme was purified approximately 3.6 fold, yielding 1.23%, using ion exchange chromatography. The molecular weight of the purified uricase was estimated to be approximately 14 kDa by SDS-PAGE. The optimum temperature and pH for uricase were determined to be 35 °C and 8–9, respectively. It was demonstrated that uricase retained up to 46% of its activity after half an hour at 40 °C and exhibited higher activity at neutral and basic pH compared to acidic pH. Its activity increased in the presence of 1 mM Mg2+, Na+, and EDTA, while it decreased by 86% in the presence of Cu2+. This study represents the first report on the production and characterization of extracellular proteolysis-resistant uricase from marine-derived Streptomyces. [ABSTRACT FROM AUTHOR]

Published

2024

37. Novel metabolite madeirone and neomarinone extracted from Streptomyces aculeoletus as marine antibiofilm and antifouling agents.

Author

Wissner, Julian L., Almeida, Joana R., Grilo, Ines R., Oliveira, Jhenifer F., Brizida, Carolina, Escobedo-Hinojosa, Wendy, Pissaridou, Panayiota, Vasquez, Marlen I., Cunha, Isabel, Sobral, Rita G., Vasconcelos, Vitor, Gaudencio, Susana P., Liu, Lingli, and Costantino, Valeria

Subjects

*METABOLITES, *STREPTOMYCES, *BIOFILMS, *MICROCOCCUS, *HIGH performance liquid chromatography

Abstract

Introduction: Biofouling poses a significant economic threat to various marine industries, leading to financial losses that can reach billions of euros annually. This study highlights the urgent need for effective alternatives to traditional antifouling agents, particularly following the global ban on organotin compounds. Material and methods: Streptomyces aculeolatus PTM-346 was isolated from sediment samples on the shores of the Madeira Archipelago, Portugal. The crude extract was fractionated using silica flash chromatography and preparative HPLC, resulting in two isolated marinone compounds: madeirone (1), a novel marinone derivative discovered in this study, and neomarinone (2). The antifouling activities of these compounds were tested against five marine bacterial species and the larvae of the mussel Mytilus galloprovincialis. Additionally, in silico and in vivo environmental toxicity evaluations of madeirone (1) and neomarinone (2) were conducted. Results: Madeirone (1) demonstrated significant antibiofilm efficacy, inhibiting Phaeobacter inhibens by up to 66%, Marinobacter hydrocarbonoclasticus by up to 60%, and Cobetia marina by up to 40%. Neomarinone (2) also exhibited substantial antibiofilm activity, with inhibition rates of up to 41% against P. inhibens, 40% against Pseudo-oceanicola batsensis, 56% against M. hydrocarbonoclasticus, 46% against C. marina, and 40% against Micrococcus luteus. The growth inhibition activity at the same concentrations of these compounds remained below 20% for the respective bacteria, highlighting their effectiveness as potent antibiofilm agents without significantly affecting bacterial viability. Additionally, both compounds showed potent effects against the settlement of Mytilus galloprovincialis larvae, with EC50 values of 1.76 μg/mL and 0.12 μg/mL for compounds (1) and (2), respectively, without impairing the viability of the targeted macrofouling species. In silico toxicity predictions and in vivo toxicity assays both support their potential for further development as antifouling agents. Conclusion: The newly discovered metabolite madeirone (1) and neomarinone (2) effectively inhibit both microand macrofouling. This distinct capability sets them apart from existing commercial antifouling agents and positions them as promising candidates for biofouling prevention. Consequently, these compounds represent a viable and environmentally friendly alternative for incorporation into paints, primers, varnishes, and sealants, offering significant advantages over traditional copper-based compounds. [ABSTRACT FROM AUTHOR]

Published

2024

38. Consortia of Streptomyces spp. triggers defense/PAMP genes during the interaction of Groundnut budnecrosis orthotospovirus in tomato.

Author

Dev, A. S. Rahul, Harish, S., Karthikeyan, G., Nivedha, M., and Sangeetha, C.

Subjects

*SEED treatment, *STREPTOMYCES, *DISEASE incidence, *CONSORTIA, *PEANUTS

Abstract

In the present study, Streptomyces spp. were isolated, characterized, and the efficacy was tested against Groundnut bud necrosis orthotospovirus (GBNV) in tomato. Among the three inoculation methods viz., pre-, post-, and simultaneous inoculation, tested for antiviral efficacy, pre-inoculation spray of the three Streptomyces spp. viz., Streptomyces mutabilis, Streptomyces rochei, and Streptomyces chrestomyceticus (SAT1, SAT4, and STR2) recorded the least disease severity index (DSI) of GBNV in tomato. In the pot culture, seed treatment of liquid consortium of three Streptomyces spp. @ 2 ml/g of seeds along with seedling dip at 10 ml/lit followed by soil drenching at 10 ml/lit on 7 days after transplanting (DAT) and foliar application at 0.5% on 15 DAT, 30 DAT, and 45 DAT recorded the least GBNV infection of 15% DSI and 16.67% DSI in trial I and II respectively. Besides, under field conditions, the disease incidence was reduced to 14.44% recording a higher yield of 76.67 t/ha in the treated plants against 63.99 t/ha in control. Upregulation of defense genes viz., PR1, PR2, PR6, WRKY, MAPKK, and NPR1 during tripartite interaction between tomato, Streptomyces, and GBNV was analyzed by qRTPCR, indicating that the consortia could decrease the virus severity through induced systemic resistance pathways. Thus, it is concluded that Streptomyces spp. can be used for the management of GBNV in tomato. [ABSTRACT FROM AUTHOR]

Published

2024

39. Streptomyces pratensis S10 Inhibits the Spread of Fusarium graminearum Invasive Hyphae and Toxisome Formation in Wheat Plants.

Author

Lifang Hu, Jing Chen, Ruimin Jia, Yan Sun, Xiaomin Dong, Shang Cao, Xihui Shen, and Yang Wang

Subjects

*GENE expression, *WHEAT, *STREPTOMYCES, *CULTIVARS, *PHLOEM

Abstract

Fusarium head blight (FHB) of wheat, mainly caused by Fusarium graminearum, leads to severe economic losses worldwide. Effective management measures for controlling FHB are not available due to a lack of resistant cultivars. Currently, the utilization of biological control a promising approach that can be used to help manage FHB. Previous studies have confirmed that Streptomyces pratensis S\O harbors excellent inhibitory effects on E graminearum. However, there is no information regarding whether invasive hyphae of E graminearum are inhibited by SIO, Thus, we investigated the effects of 310 on E graininearum strain PH-1 hypha extension, toxisome formation, and TRI5 gene expression on wheat plants via microscopic observation. The results showed that 10 effectively inhibited the spread of K graminearum hyphae along the rachis, restricting the infection of neighboring florets via the phloem. In the presence of S 10, the hyphal growth is impeded by the formation of dense cell wall thickenings in the racllis internode surrounding the E graminearum infection site, avoiding cell plasmolysis and collapse. We further demonstrated that SIO largely prevented cell-to-cell invasion of fungal hyphae inside wheat coleoptiles using a constitutively green fluorescence protein-expressing E graminectrum strain, PH - 1. Importantly, S. pratensis S10 inhibited toxisome formation and TR/5 gene expression in wheat plants during infection. Collectively, these findings indicate that S. pratensis S\O prevents the spread of E graminearum invasive hyphae via the rachis. [ABSTRACT FROM AUTHOR]

Published

2024

40. 海草床盐生植物根际土壤可培养细菌 多样性及抑菌活性研究.

Author

陈望安, 李蜜, 黎芳婷, and 高程海

Subjects

*BACILLUS (Bacteria), *MICROBACTERIUM, *METHICILLIN-resistant staphylococcus aureus, *SHIGELLA, *SEAGRASSES

Abstract

The purpose of this study was to investigate the novelty and particularly of the culturable bacteria in seagrass bed and study its antibacterial activity crude extracts of the metabolites. A total of nine rhizosphere soil samples were collected from the seagrass bed ecosystems in Pearl Bay and Yuzhouping, Fangchenggang City. Five different isolation media were used to isolate and purify the culturable bacteria using the dilution spread plate method. The bacterial species were identified through PCR amplification and 16S rRNA sequencing. The antibacterial activity against four human pathogenic bacteria (methicillin-resistant Staphylococcus aureus, S. epidermidis, S. aureus and Acinetobacter baumannii) were screened with Kirby-Bauer method. The results were as follows: (1) A total of 42 culturable bacteria were isolated, belonging to 14 genera and 13 families, which included Streptomyces, Vibrio, Bacillus, Shewanella, Microbacterium, Brevibacterium, Staphylococcus, Sphingomonas, Rothia, Psychrobacter, Pseudonocardia, Photobacterium, Halomonas, and Shigella. The genus Streptomyces was the dominant bacterium. (2) Antibacterial activity showed that six bacteria exhibited strong inhibitory activity against at least two or more human pathogenic bacteria, which included Vibrio (1 strain), Rothia (1 strain), and Streptomyces (4 strains). The studies show that the rhizosphere soil microbial resources of halophytes in the seagrass bed in Fangchenggang sea area are novel and unique, and Streptomyces has a strong antibacterial activity, which provides a new source for the research and development of new antibiotics drugs. [ABSTRACT FROM AUTHOR]

Published

2024

41. Streptomyces mahasarakhamensis sp. nov., an Endophytic Actinobacterium Isolated from Jasmine Rice and its Potential as plant Growth Promoter.

Author

Sukpanoa, Sudarat, Kaewkla, Onuma, Suriyachadkun, Chanwit, Papayrata, Chanakran, Klankeo, Piriya, and Franco, Christopher Milton Mathew

Abstract

Two endophytic actinobacteria, strains MK5T and MK7, were isolated from the surface-sterilized root of Jasmine rice (Oryza sativa KDML 105). These strains were aerobic actinobacteria with a well-developed substrate and aerial mycelia that formed spiral spore chains. The type strains that shared the high 16S rRNA gene sequence similarity with both strains were Streptomyces naganishii NBRC 12892T (99.4%), “Streptomyces griseicoloratus” TRM S81-3T (99.2%), and Streptomyces spiralis NBRC 14215T (98.9%). Strains MK5T and MK7 are the same species sharing a digital DNA–DNA hybridization (dDDH) value of 95.3% and a 16S rRNA gene sequence similarity of 100%. Chemotaxonomic data confirmed the affiliation of strains MK5T and MK7 to the genus Streptomyces. Strains MK5T and MK7 contained MK-9(H4) as a major menaquinone; the whole-cell sugar of both strains was galactose and glucose. The strain MK5T shared 93.4% average nucleotide identity (ANI)-Blast, 95.5% ANI-MUMmer, 93% average amino acid identity, and 61.3% dDDH with S. spiralis NBRC 14215T. The polyphasic approach confirmed that strain MK5T represents a novel species, and the name Streptomyces mahasarakhamensis sp. nov. is proposed. The type strain is MK5T (= TBRC 17754 = NRRL B-65683). Genome mining, using an in silico approach and searching biosynthesis gene clusters of strains MK5T and MK7, revealed that the genomes contained genes encoding proteins relating to plant growth promotion, bioactive compounds, and beneficial enzymes. Strains MK5T and MK7 could produce indole acetic acid and solubilize phosphate in vitro. [ABSTRACT FROM AUTHOR]

Published

2024

42. Development of bioinsecticide based on Streptomyces griseoflavus PAL114 for control of black bean aphids Aphis fabae.

Author

Benbelkhir, Fatma Zohra, Allali, Khadidja, Benadjila, Abderrahmane, Goudjal, Yacine, Medjekal, Samir, and Zamoum, Miyada

Subjects

*BLACK bean, *FAVA bean, *STREPTOMYCES, *ACTINOBACTERIA, *SOIL amendments, *APHIDS

Abstract

This research highlights the efficiency of a bioinsecticide based on Streptomyces griseoflavus PAL114 in controlling black bean aphids and its effect on fava beans. Three actinobacterial strains were tested in vitro for their aphicidal activity. The PAL114 strain was then formulated in talc powder and tested again. Formulation processes were performed with four spore suspension densities (102, 104, 106 and 108 spore ml−1) at a rate of 25 ml per 100 g of talc powder. Furthermore, the in vivo effect of bioinsecticide on fava bean plants was studied in pot experiments using two application methods: spray and spray + soil amendment. The results showed that only the PAL114 strain had a highly significant effect on mortality (p =.001). Their high-density formulations at 106 and 108 spore ml−1 induced very highly significant activity (p <.001) for both, with no influence difference exceeding 90% after 58 h. In contrast, the other low-density formulations at 102 and 104 spore ml−1 had no significant effect (p =.322 and p = 1.000, respectively). There was no adverse effect of the bioinsecticide on fava bean; instead, there was an improvement in growth, especially when the spray application was combined with soil amendment. The present study opens up prospects for field studies on the biocontrol of this crop pest. [ABSTRACT FROM AUTHOR]

Published

2024

43. Editing Streptomyces genome using target AID system fused with UGI‐degradation tag.

Author

Apriliana, Pamella, Kahar, Prihardi, Kashiwagi, Norimasa, Kondo, Akihiko, and Ogino, Chiaki

Subjects

*CRISPRS, *CYTIDINE deaminase, *STREPTOMYCES coelicolor, *GENE expression, *SEA lamprey, *IMMUNOGLOBULIN class switching

Abstract

The utilization of Streptomyces as a microbial chassis for developing innovative drugs and medicinal compounds showcases its capability to produce bioactive natural substances. Recent focus on the clustered regularly interspaced short palindromic repeat (CRISPR) technology highlights its potential in genome editing. However, applying CRISPR technology in certain microbial strains, particularly Streptomyces, encounters specific challenges. These challenges include achieving efficient gene expression and maintaining genetic stability, which are critical for successful genome editing. To overcome these obstacles, an innovative approach has been developed that combines several key elements: activation‐induced cytidine deaminase (AID), nuclease‐deficient cas9 variants (dCas9), and Petromyzon marinus cytidine deaminase 1 (PmCDA1). In this study, this novel strategy was employed to engineer a Streptomyces coelicolor strain. The target gene was actVA‐ORF4 (SCO5079), which is involved in actinorhodin production. The engineering process involved introducing a specific construct [pGM1190‐dcas9‐pmCDA‐UGI‐AAV‐actVA‐ORF4 (SCO5079)] to create a CrA10 mutant strain. The resulting CrA10 mutant strain did not produce actinorhodin. This outcome highlights the potential of this combined approach in the genetic manipulation of Streptomyces. The failure of the CrA10 mutant to produce actinorhodin conclusively demonstrates the success of gene editing at the targeted site, affirming the effectiveness of this method for precise genetic modifications in Streptomyces. [ABSTRACT FROM AUTHOR]

Published

2024

44. Bioactive Naphthoquinone and Phenazine Analogs from the Endophytic Streptomyces sp. PH9030 as α-Glucosidase Inhibitors.

Author

Ma, Qingxian, Zhong, Yani, Huang, Pingzhi, Li, Aijie, Jiang, Ting, Jiang, Lin, Yang, Hao, Wang, Zhong, Wu, Guangling, Huang, Xueshuang, Pu, Hong, and Liu, Jianxin

Subjects

*METHICILLIN-resistant staphylococcus aureus, *NAPHTHOQUINONE, *MOLECULAR docking, *STREPTOMYCES, *MOLECULAR dynamics, *GLYCOSIDASE inhibitors

Abstract

A talented endophytic Streptomyces sp. PH9030 is derived from the medicinal plant Kadsura coccinea (Lem.) A.C. Smith. The undescribed naphthoquinone naphthgeranine G (5) and seven previously identified compounds, 6–12, were obtained from Streptomyces sp. PH9030. The structure of 5 was identified by comprehensive examination of its HRESIMS, 1D NMR, 2D NMR and ECD data. The inhibitory activities of all the compounds toward α-glucosidase and their antibacterial properties were investigated. The α-glucosidase inhibitory activities of 5, 6, 7 and 9 were reported for the first time, with IC50 values ranging from 66.4 ± 6.7 to 185.9 ± 0.2 μM, as compared with acarbose (IC50 = 671.5 ± 0.2 μM). The molecular docking and molecular dynamics analysis of 5 with α-glucosidase further indicated that it may have a good binding ability with α-glucosidase. Both 9 and 12 exhibited moderate antibacterial activity against methicillin-resistant Staphylococcus aureus, with minimum inhibitory concentration (MIC) values of 16 μg/mL. These results indicate that 5, together with the naphthoquinone scaffold, has the potential to be further developed as a possible inhibitor of α-glucosidase. [ABSTRACT FROM AUTHOR]

Published

2024

45. Characteristics and kinetics of thermophilic actinomycetesʼ amylase production on agro-wastes and its application for ethanol fermentation.

Author

El-Sayed, Mohamed H., Gomaa, Abd El-Rahman F., Atta, Omar Mohammad, and Hassane, Abdallah M. A.

Subjects

*AMYLASES, *ACTINOBACTERIA, *SUSTAINABILITY, *FERMENTATION, *WHEAT straw, *ETHANOL, *AMYLOLYSIS

Abstract

Thermophilic actinomycetes are commonly found in extreme environments and can thrive and adapt to extreme conditions. These organisms exhibit substantial variation and garnered significant interest due to their remarkable enzymatic activities. This study evaluated the potential of Streptomyces griseorubens NBR14 and Nocardiopsis synnemataformans NBRM9 strains to produce thermo-stable amylase via submerged fermentation using wheat and bean straw. The Box-Behnken design was utilized to determine the optimum parameters for amylase biosynthesis. Subsequently, amylase underwent partial purification and characterization. Furthermore, the obtained hydrolysate was applied for ethanol fermentation using Saccharomyces cerevisiae. The optimal parameters for obtaining the highest amylase activity by NBR14 (7.72 U/mL) and NBRM9 (26.54 U/mL) strains were found to be 40 and 30 °C, pH values of 7, incubation time of 7 days, and substrate concentration (3 and 2 g/100 mL), respectively. The NBR14 and NBRM9 amylase were partially purified, resulting in specific activities of 251.15 and 144.84 U/mg, as well as purification factors of 3.91 and 2.69-fold, respectively. After partial purification, the amylase extracted from NBR14 and NBRM9 showed the highest activity level at pH values of 9 and 7 and temperatures of 50 and 60 °C, respectively. The findings also indicated that the maximum velocity (Vmax) for NBR14 and NBRM9 amylase were 57.80 and 59.88 U/mL, respectively, with Km constants of 1.39 and 1.479 mM. After 48 h, bioethanol was produced at concentrations of 5.95 mg/mL and 9.29 mg/mL from hydrolyzed wheat and bean straw, respectively, through fermentation with S. cerevisiae. Thermophilic actinomycetes and their α-amylase yield demonstrated promising potential for sustainable bio-ethanol production from agro-byproducts. [ABSTRACT FROM AUTHOR]

Published

2024

46. Bioproducts derived from <italic>Bacillus stercoris</italic> isolate B.PNR1 and <italic>Streptomyces</italic> sp. isolate S.PNR29 for enhanced plant growth and disease control in tomato.

Author

Kawicha, Praphat, Pengproh, Rattana, Thanyasiriwat, Thanwanit, Sangdee, Kusavadee, and Sangdee, Aphidech

Subjects

*BIOLOGICAL products, *PLANT diseases, *PLANT growth, *TOMATOES, *SUSTAINABLE agriculture, *SUSTAINABILITY, *WILT diseases

Abstract

This study aims to develop a wettable formulation bioproduct from antagonistic bacteria, Bacillus stercoris isolate B.PNR1, and Streptomyces sp. isolate S.PNR29, targeting Fusarium oxysporum f.sp. lycopersici (Fol), the cause of Fusarium wilt disease in tomatoes, while also promoting plant growth. The survivability of bacterial cells in the product was assessed over a 180-day period at 4°C and 28°C. The bioproducts demonstrated significant control of Fusarium wilt disease, with B. stercoris isolate B.PNR1 bioproducts exhibiting superior disease control percentages compared to Streptomyces sp. isolate S.PNR29 bioproducts and commercial alternatives. Additionally, the bioproducts positively influenced tomato seed germination and seedling growth, with Streptomyces sp. isolate S.PNR29 bioproducts showing better growth performance in terms of plant length, weight measurements, and seed germination. In conclusion, B. stercoris isolate B.PNR1 and Streptomyces sp. isolate S.PNR29 bioproducts emerge as promising biocontrol agents, showcasing sustained efficacy against Fol and significant positive impacts on plant growth, thereby highlighting their potential for sustainable agriculture practices. [ABSTRACT FROM AUTHOR]

Published

2024

47. Discovery of anti-Mycobacterium tuberculosis desertomycins from Streptomyces flavofungini TRM90047 based on genome mining and HSQC-TOCSY.

Author

Wang, Lei, Reheman, Aikebaier, and Wan, Chuanxing

Subjects

*MYCOBACTERIUM tuberculosis, *STREPTOMYCES, *TUBERCULOSIS, *QUANTUM correlations, *MOLECULAR docking

Abstract

Tuberculosis caused by Mycobacterium tuberculosis (M. tb) is a major public health problem with high morbidity and mortality worldwide. In our previous study, we found that a fermentation product of Streptomyces flavofungini TRM90047 exhibited anti-M. tb activity and decreased the expression level of several genes, including rpsL, Rplc and ClpC1. Guided by heteronuclear single quantum correlation-total correlation spectroscopy (HSQC-TOCSY) fingerprints and genome mining, we isolated two new 44-membered macrolides, desertomycin 44-1 (1) and desertomycin 44-2 (2), together with known desertomycin A (3) from S. flavofungini TRM90047. Three desertomycins showed anti-M. tb activity. The EC50 values of desertomycin A, desertomycin 44-1 and desertomycin 44-2 were 25 µg/mL, 25 µg/mL and 50 µg/mL, respectively. Molecular docking analyses revealed that the isolated desertomycins bound well to the RPSL, RPLC and CLPC1 proteins. In the present study, we describe the discovery of new anti-M. tb compounds guided by genome mining, HSQC-TOCSY and anti-M. tb bioassays. [ABSTRACT FROM AUTHOR]

Published

2024

48. Prophage induction can facilitate the in vitro dispersal of multicellular Streptomyces structures.

Author

Jaffal, Hoda, Kortebi, Mounia, Misson, Pauline, Tavares, Paulo, Ouldali, Malika, Leh, Hervé, Lautru, Sylvie, Lioy, Virginia S., Lecointe, François, and Bury-Moné, Stéphanie G.

Subjects

*STREPTOMYCES, *MOBILE genetic elements, *BACTERIAL physiology, *SOIL ecology, *BACTERIOPHAGES

Abstract

Streptomyces are renowned for their prolific production of specialized metabolites with applications in medicine and agriculture. These multicellular bacteria present a sophisticated developmental cycle and play a key role in soil ecology. Little is known about the impact of Streptomyces phage on bacterial physiology. In this study, we investigated the conditions governing the expression and production of "Samy," a prophage found in Streptomyces ambofaciens ATCC 23877. This siphoprophage is produced simultaneously with the activation of other mobile genetic elements. Remarkably, the presence and production of Samy increases bacterial dispersal under in vitro stress conditions. Altogether, this study unveiled a new property of a bacteriophage infection in the context of multicellular aggregate dynamics. Little is known about the impact of phages on Streptomyces physiology. In this study, induction of the prophage 'Samy' was found to enhance the dispersal of multicellular aggregates of Streptomyces ambofaciens bacteria in response to stress, likely promoting lineage propagation. [ABSTRACT FROM AUTHOR]

Published

2024

49. Discovery of antimalarial drugs from secondary metabolites in actinomycetes culture library.

Author

Teklemichael, Awet Alem, Teshima, Aiko, Hirata, Asahi, Akimoto, Momoko, Taniguchi, Mayumi, Khodakaramian, Gholam, Fujimura, Takashi, Tokumasu, Fuyuki, Arakawa, Kenji, and Mizukami, Shusaku

Subjects

*METABOLITES, *ACTINOBACTERIA, *ETHYL acetate, *CYTOTOXINS, *NATURAL products

Abstract

Background: Natural products play a key role as potential sources of biologically active substances for the discovery of new drugs. This study aimed to identify secondary metabolites from actinomycete library extracts that are potent against the asexual stages of Plasmodiumfalciparum (P.falciparum). Methods: Secondary metabolites from actinomycete library extracts were isolated from culture supernatants by ethyl acetate extraction. Comprehensive screening was performed to identify novel antimalarial compounds from the actinomycete library extracts (n = 28). The antimalarial activity was initially evaluated in vitro against chloroquine/mefloquine-sensitive (3D7) and-resistant (Dd2) lines of P.falciparum. The cytotoxicity was then evaluated in primary adult mouse brain (AMB) cells. Results: Out of the 28 actinomycete extracts, 17 showed parasite growth inhibition > 50% at a concentration of 50 µg/mL, nine were identified with an IC50 value < 10 µg/mL, and seven suppressed the parasite significantly with an IC50 value < 5 µg/mL. The extracts from Streptomycesaureus strains HUT6003 (Extract ID number: 2), S.antibioticus HUT6035 (8), and Streptomyces sp. strains GK3 (26) and GK7 (27), were found to have the most potent antimalarial activity with IC50 values of 0.39, 0.09, 0.97, and 0.36 µg/mL (against 3D7), and 0.26, 0.22, 0.72, and 0.21 µg/mL (against Dd2), respectively. Among them, Streptomycesantibioticus strain HUT6035 (8) showed the highest antimalarial activity with an IC50 value of 0.09 µg/mL against 3D7 and 0.22 µg/mL against Dd2, and a selective index (SI) of 188 and 73.7, respectively. Conclusion: Secondary metabolites obtained from the actinomycete extracts showed promising antimalarial activity in vitro against 3D7 and Dd2 cell lines of P.falciparum with minimal toxicity. Therefore, secondary metabolites obtained from actinomycete extracts represent an excellent starting point for the development of antimalarial drug leads. [ABSTRACT FROM AUTHOR]

Published

2024

50. Green synthesis of zinc oxide nanoparticles (ZnO-NPs) by Streptomyces baarnensis and its active metabolite (Ka): a promising combination against multidrug-resistant ESKAPE pathogens and cytotoxicity.

Author

Kalaba, Mohamed H., El-Sherbiny, Gamal M., Ewais, Emad A., Darwesh, Osama M., and Moghannem, Saad A.

Subjects

*ZINC oxide synthesis, *CYTOTOXINS, *STREPTOMYCES, *PATHOGENIC bacteria, *GRAM-negative bacteria, *ZINC oxide

Abstract

Various eco-friendly techniques are being researched for synthesizing ZnO-NPs, known for their bioactivity. This study aimed at biosynthesizing ZnO-NPs using Streptomyces baarnensis MH-133, characterizing their physicochemical properties, investigating antibacterial activity, and enhancement of their efficacy by combining them with a water-insoluble active compound (Ka) in a nanoemulsion form. Ka is a pure compound of 9-Ethyl-1,4,6,9,10-pentahydroxy-7,8,9,10-tetrahydrotetracene-5,12-dione obtained previously from our strain of Streptomyces baarnensis MH-133. Biosynthesized ZnO-NPs employing Streptomyces baarnensis MH-133 filtrate and zinc sulfate (ZnSO4.7H2O) as a precursor were purified and characterized by physicochemical investigation. High-resolution-transmission electron microscopy (HR-TEM) verified the effective biosynthesis of ZnO-NPs (size < 12 nm), whereas dynamic light scattering (DLS) analysis showed an average size of 17.5 nm. X-ray diffraction (XRD) exhibited characteristic diffraction patterns that confirmed crystalline structure. ZnO-NPs efficiently inhibited both Gram-positive and Gram-negative bacteria (MICs: 31.25–125 µg/ml). The pure compound (Ka) was combined with ZnO-NPs to improve effectiveness and reduce dose using checkerboard microdilution. Niteen treatments of Ka and ZnO-NPs combinations obtained by checkerboard matrix inhibited Klebsiella pneumonia. Eleven combinations had fractional inhibitory concentration index (FICi) between 1.03 and 2, meaning indifferent, another five combinations resulted from additive FICi (0.625–1) and only one combination with FICi of 0.5, indicating synergy. In the case of methicillin-resistant S. aureus (MRSA), Ka-ZnO-NPs combinations yielded 23 treatments with varying degrees of interaction. The results showed eleven treatments with indifferent interaction, eight additive interactions, and two synergies with FICi of 0.5 and 0.375. The combinations that exhibited synergy action were transformed into a nanoemulsion form to improve their solubility and bioavailability. The HR-TEM analysis of the nanoemulsion revealed spherical oil particles with a granulated core smaller than 200 nm and no signs of aggregation. Effective dispersion was confirmed by DLS analysis which indicated that Ka-ZnO-NPs nanoemulsion droplets have an average size of 53.1 nm and a polydispersity index (PI) of 0.523. The killing kinetic assay assessed the viability of methicillin-resistant Staphylococcus aureus (MRSA) and K. pneumonia post-treatment with Ka-ZnO-NPs combinations either in non-formulated or nanoemulsion form. Results showed Ka-ZnO-NPs combinations show concentration and time-dependent manner, with higher efficacy in nanoemulsion form. The findings indicated that Ka-ZnO-NPs without formulation at MIC values killed K. pneumonia after 24 h but not MRSA. Our nanoemulsion loaded with the previously mentioned combinations at MIC value showed bactericidal effect at MIC concentration of Ka-ZnO-NPs combination after 12 and 18 h of incubation against MRSA and K. pneumonia, respectively, compared to free combinations. At half MIC value, nanoemulsion increased the activity of the combinations to cause a bacteriostatic effect on MRSA and K. pneumonia after 24 h of incubation. The free combination showed a bacteriostatic impact for 6 h before the bacteria regrew to increase log10 colony forming unit (CFU)/ml over the initial level. Similarly, the cytotoxicity study revealed that the combination in nanoemulsion form decreased the cytotoxicity against kidney epithelial cells of the African green monkey (VERO) cell line. The IC50 for Ka-ZnO-NPs non-formulated treatment was 8.17/1.69 (µg/µg)/ml, but in nano-emulsion, it was 22.94 + 4.77 (µg/µg)/mL. In conclusion, efficient Ka-ZnO-NPs nanoemulsion may be a promising solution for the fighting of ESKAPE pathogenic bacteria according to antibacterial activity and low toxicity. [ABSTRACT FROM AUTHOR]

Published

2024