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A Novel Resistance Pathway for Calcineurin Inhibitors in the Human-Pathogenic Mucorales Mucor circinelloides.

Publication ,  Journal Article
Vellanki, S; Billmyre, RB; Lorenzen, A; Campbell, M; Turner, B; Huh, EY; Heitman, J; Lee, SC
Published in: Mbio
January 28, 2020

Mucormycosis is an emerging lethal fungal infection in immunocompromised patients. Mucor circinelloides is a causal agent of mucormycosis and serves as a model system to understand genetics in Mucorales. Calcineurin is a conserved virulence factor in many pathogenic fungi, and calcineurin inhibition or deletion of the calcineurin regulatory subunit (CnbR) in Mucor results in a shift from hyphal to yeast growth. We analyzed 36 calcineurin inhibitor-resistant or bypass mutants that exhibited hyphal growth in the presence of calcineurin inhibitors or in the yeast-locked cnbRΔ mutant background without carrying any mutations in known calcineurin components. We found that a majority of the mutants had altered sequence in a gene, named here bycA (bypass of calcineurin). bycA encodes an amino acid permease. We verified that both the bycAΔ single mutant and the bycAΔ cnbRΔ double mutant are resistant to calcineurin inhibitor FK506, thereby demonstrating a novel mechanism of resistance against calcineurin inhibitors. We also found that the level of expression of bycA was significantly higher in the wild-type strain treated with FK506 and in the cnbRΔ mutants but was significantly lower in the wild-type strain without FK506 treatment. These findings suggest that bycA is a negative regulator of hyphal growth and/or a positive regulator of yeast growth in Mucor and that calcineurin suppresses expression of the bycA gene at the mRNA level to promote hyphal growth. BycA is involved in the Mucor hypha-yeast transition as our data demonstrate positive correlations among bycA expression, protein kinase A activity, and Mucor yeast growth. Also, calcineurin, independently of its role in morphogenesis, contributes to virulence traits, including phagosome maturation blockade, host cell damages, and proangiogenic growth factor induction during interactions with hosts.IMPORTANCEMucor is intrinsically resistant to most known antifungals, which makes mucormycosis treatment challenging. Calcineurin is a serine/threonine phosphatase that is widely conserved across eukaryotes. When calcineurin function is inhibited in Mucor, growth shifts to a less virulent yeast growth form, which makes calcineurin an attractive target for development of new antifungal drugs. Previously, we identified two distinct mechanisms through which Mucor can become resistant to calcineurin inhibitors involving Mendelian mutations in the gene for FKBP12, including mechanisms corresponding to calcineurin A or B subunits and epimutations silencing the FKBP12 gene. Here, we identified a third novel mechanism where loss-of-function mutations in the amino acid permease corresponding to the bycA gene contribute to resistance against calcineurin inhibitors. When calcineurin activity is absent, BycA can activate protein kinase A (PKA) to promote yeast growth via a cAMP-independent pathway. Our data also show that calcineurin activity contributes to host-pathogen interactions primarily in the pathogenesis of Mucor.

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Published In

Mbio

DOI

EISSN

2150-7511

Publication Date

January 28, 2020

Volume

11

Issue

1

Location

United States

Related Subject Headings

  • Virulence Factors
  • Virulence
  • RNA, Messenger
  • Mutation
  • Mucormycosis
  • Mucor
  • Models, Biological
  • Microbial Sensitivity Tests
  • Humans
  • Host-Pathogen Interactions
 

Citation

APA
Chicago
ICMJE
MLA
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Vellanki, S., Billmyre, R. B., Lorenzen, A., Campbell, M., Turner, B., Huh, E. Y., … Lee, S. C. (2020). A Novel Resistance Pathway for Calcineurin Inhibitors in the Human-Pathogenic Mucorales Mucor circinelloides. Mbio, 11(1). https://doi.org/10.1128/mBio.02949-19
Vellanki, Sandeep, R Blake Billmyre, Alejandra Lorenzen, Micaela Campbell, Broderick Turner, Eun Young Huh, Joseph Heitman, and Soo Chan Lee. “A Novel Resistance Pathway for Calcineurin Inhibitors in the Human-Pathogenic Mucorales Mucor circinelloides.Mbio 11, no. 1 (January 28, 2020). https://doi.org/10.1128/mBio.02949-19.
Vellanki S, Billmyre RB, Lorenzen A, Campbell M, Turner B, Huh EY, et al. A Novel Resistance Pathway for Calcineurin Inhibitors in the Human-Pathogenic Mucorales Mucor circinelloides. Mbio. 2020 Jan 28;11(1).
Vellanki, Sandeep, et al. “A Novel Resistance Pathway for Calcineurin Inhibitors in the Human-Pathogenic Mucorales Mucor circinelloides.Mbio, vol. 11, no. 1, Jan. 2020. Pubmed, doi:10.1128/mBio.02949-19.
Vellanki S, Billmyre RB, Lorenzen A, Campbell M, Turner B, Huh EY, Heitman J, Lee SC. A Novel Resistance Pathway for Calcineurin Inhibitors in the Human-Pathogenic Mucorales Mucor circinelloides. Mbio. 2020 Jan 28;11(1).

Published In

Mbio

DOI

EISSN

2150-7511

Publication Date

January 28, 2020

Volume

11

Issue

1

Location

United States

Related Subject Headings

  • Virulence Factors
  • Virulence
  • RNA, Messenger
  • Mutation
  • Mucormycosis
  • Mucor
  • Models, Biological
  • Microbial Sensitivity Tests
  • Humans
  • Host-Pathogen Interactions