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Yinlan Bai

Researcher at Albany Medical College

Publications -  5
Citations -  456

Yinlan Bai is an academic researcher from Albany Medical College. The author has contributed to research in topics: Cyclase & Streptococcus pneumoniae. The author has an hindex of 4, co-authored 5 publications receiving 381 citations.

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Cyclic Di-AMP Impairs Potassium Uptake Mediated by a Cyclic Di-AMP Binding Protein in Streptococcus pneumoniae

TL;DR: A direct c-di-AMP-mediated signaling pathway that regulates pneumococcal potassium uptake is established and is established as a direct interaction between CabP and SPD_0076 and the efficiency of potassium uptake were impaired by elevated c- di-AMP in pneumococci.
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Two DHH subfamily 1 proteins in Streptococcus pneumoniae possess cyclic di-AMP phosphodiesterase activity and affect bacterial growth and virulence.

TL;DR: It is shown that c-di-AMP homeostasis is essential for pneumococcal biology and disease and that both Pde1 and Pde2 played roles in bacterial growth, resistance to UV treatment, and virulence in a mouse pneumonia model.
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Deletion of the cyclic di‐AMP phosphodiesterase gene (cnpB) in Mycobacterium tuberculosis leads to reduced virulence in a mouse model of infection

TL;DR: It is demonstrated that a protein encoded by Rv2837c (cnpB) possesses c‐di‐AMP phosphodiesterase activity and cleaves c‐ di‐AMP exclusively to AMP, which indicates that deletion of cnpB results in attenuated virulence, which is correlated with elevated c‐Di‐AMP levels.
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Mycobacterium tuberculosis Rv3586 (DacA) is a diadenylate cyclase that converts ATP or ADP into c-di-AMP.

TL;DR: The results showed that Mycobacterium tuberculosis Rv3586 (DacA) was mainly a diadenylate cyclase, which resembles DisA, and it was demonstrated that DacA existed as an octamer, with the N-terminal domain contributing to tetramerization and the C- terminal domain providing additional dimerization.