Antibiotic GE2270
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Antibiotic GE2270

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Antibiotic GE2270 is a thiopeptide antibiotic produced by Planobispora rosea. It has antibacterial activity against Gram-positive bacteria and a few Gram-negative bacteria. It is particularly active against anaerobes.

Category
Functional Peptides
Catalog number
BAT-013157
Synonyms
Thiocillin GE2270
Appearance
Lyophilized Powder
Purity
>85%
Sequence
SCNCVCGFCCSCSP
Storage
Store at -20°C
1. Antibacterial Thiopeptide GE2270-Congeners from Nonomuraea jiangxiensis
Kuan-Chieh Ching, et al. Molecules. 2022 Dec 23;28(1):101. doi: 10.3390/molecules28010101.
Thiopeptides are macrocyclic natural products with potent bioactivity. Nine new natural thiopeptides (1-9) were obtained from a Nonomuraea jiangxiensis isolated from a terrestrial soil sample collected in Singapore. Even though some of these compounds were previously synthesized or isolated from engineered strains, herein we report the unprecedented isolation of these thiopeptides from a native Nonomuraea jiangxiensis. A comparison with the literature and a detailed analysis of the NMR and HRMS of compounds 1-9 was conducted to assign their chemical structures. The structures of all new compounds were highly related to the thiopeptide antibiotics GE2270, with variations in the substituents on the thiazole and amino acid moieties. Thiopeptides 1-9 exhibited a potent antimicrobial activity against the Gram-positive bacteria, Staphylococcus aureus with MIC90 values ranging from 2 µM to 11 µM. In addition, all compounds were investigated for their cytotoxicity against the human cancer cell line A549, none of the compounds were cytotoxic.
2. Heterologous expression of the thiopeptide antibiotic GE2270 from Planobispora rosea ATCC 53733 in Streptomyces coelicolor requires deletion of ribosomal genes from the expression construct
Katrin Flinspach, Claudia Kapitzke, Arianna Tocchetti, Margherita Sosio, Alexander K Apel PLoS One. 2014 Mar 5;9(3):e90499. doi: 10.1371/journal.pone.0090499. eCollection 2014.
GE2270 is a thiopeptide antibiotic generated by extensive posttranslational modifications of a ribosomally generated precursor peptide. Thiopeptides are especially active against Gram-positive bacteria, including methicillin resistant Staphylococcus aureus (MRSA). In this study the GE2270 biosynthetic gene cluster (pbt) from Planobispora rosea ATCC 53733 was successfully expressed in the heterologous host strain Streptomyces coelicolor M1146. Notably, exconjugants containing the pbt gene cluster could only be obtained after deletion of the major part of the ribosomal genes flanking the gene cluster. This is a striking example that genes belonging to primary metabolism can prevent the successful conjugative transfer of DNA from phylogenetic distant species and thus complicate heterologous expression of secondary metabolite gene clusters. GE2270 production in the heterologous producer strain increased after introduction of the constitutive ermE* promoter upstream of the GE2270 resistance gene tuf from P. rosea. Insertion of the inducible tcp830 promoter resulted in inducible GE2270 production. When the regulatory gene pbtR was deleted, the resulting strain ceased to produce GE2270, suggesting an essential role of PbtR as a putative transcriptional activator of GE2270 expression.
3. Antibiotic GE2270 a: a novel inhibitor of bacterial protein synthesis. I. Isolation and characterization
E Selva, G Beretta, N Montanini, G S Saddler, L Gastaldo, P Ferrari, R Lorenzetti, P Landini, F Ripamonti, B P Goldstein J Antibiot (Tokyo). 1991 Jul;44(7):693-701. doi: 10.7164/antibiotics.44.693.
A novel antibiotic, GE2270 A, was isolated from the fermentation broth of a strain of Planobispora rosea. The product was found to inhibit bacterial protein synthesis. Structural characteristics showed similarities between GE2270 A and thiazolyl peptides such as micrococcin which is known to inhibit protein synthesis by acting directly on the ribosome. Despite this similarity GE2270 A showed functional analogy to kirromycin-like antibiotics and pulvomycin, as its molecular target was found to be elongation factor Tu (EF-Tu). GE2270 A is active against Gram-positive microorganism and anaerobes and differs from the other EF-Tu inhibitors in its spectrum of antimicrobial activity.
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