Crosstalk of TetR-like regulator SACE_4839 and a nitrogen regulator for erythromycin biosynthesis
TetR family transcriptional regulators (TFRs) are widespread in actinomycetes, which exhibit diverse regulatory modes in antibiotic biosynthesis. Nitrogen regulators play vital roles in modulation of primary and secondary metabolism. However, crosstalk between TFR and nitrogen regulator has rarely b...
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Veröffentlicht in: | Applied microbiology and biotechnology 2022-10, Vol.106 (19-20), p.6551-6566 |
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Sprache: | eng |
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Zusammenfassung: | TetR family transcriptional regulators (TFRs) are widespread in actinomycetes, which exhibit diverse regulatory modes in antibiotic biosynthesis. Nitrogen regulators play vital roles in modulation of primary and secondary metabolism. However, crosstalk between TFR and nitrogen regulator has rarely been reported in actinomycetes. Herein, we demonstrated that a novel TFR, SACE_4839, was negatively correlated with erythromycin yield in
Saccharopolyspora erythraea
A226. SACE_4839 indirectly suppressed erythromycin synthetic gene
eryAI
and resistance gene
ermE
and directly inhibited its adjacent gene
SACE_4838
encoding a homologue of nitrogen metabolite repression (NMR) regulator NmrA (herein named NmrR). The SACE_4839-binding sites within
SACE_4839-nmrR
intergenic region were identified. NmrR positively controlled erythromycin biosynthesis by indirectly stimulating
eryAI
and
ermE
and directly repressing
SACE_4839
. NmrR was found to affect growth viability under the nitrogen source supply. Furthermore, NmrR directly repressed glutamine and glutamate utilization-related genes
SACE_1623
,
SACE_5070
and
SACE_5979
but activated nitrate utilization-associated genes
SACE_1163
,
SACE_4070
and
SACE_4912
as well as nitrite utilization-associated genes
SACE_1476
and
SACE_4514
. This is the first reported NmrA homolog for modulating antibiotic biosynthesis and nitrogen metabolism in actinomycetes. Moreover, combinatorial engineering of
SACE_4839
and
nmrR
in the high-yield
S. erythraea
WB resulted in a 68.8% increase in erythromycin A production. This investigation deepens the understanding of complicated regulatory network for erythromycin biosynthesis.
Key points
• SACE_4839 and NmrR had opposite contributions to erythromycin biosynthesis.
• NmrR was first identified as a homolog of another nitrogen regulator NmrA.
• Cross regulation between SACE_4839 and NmrR was revealed. |
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ISSN: | 0175-7598 1432-0614 |
DOI: | 10.1007/s00253-022-12153-0 |