Genetic and behavioral adaptation of Candida parapsilosis to the microbiome of hospitalized infants revealed by in situ genomics, transcriptomics, and proteomics

Patrick T. West; Samantha L. Peters; Matthew R. Olm; Feiqiao B. Yu; Haley Gause; Yue Clare Lou; Brian A. Firek; Robyn Baker; Alexander D. Johnson; Michael J. Morowitz; Robert L. Hettich; Jillian F. Banfield

doi:10.1186/s40168-021-01085-y

Genetic and behavioral adaptation of Candida parapsilosis to the microbiome of hospitalized infants revealed by in situ genomics, transcriptomics, and proteomics

Patrick T. West, Samantha L. Peters, Matthew R. Olm, Feiqiao B. Yu, Haley Gause, Yue Clare Lou, Brian A. Firek, Robyn Baker, Alexander D. Johnson, Michael J. Morowitz, Robert L. Hettich, Jillian F. Banfield

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13 Citations (Scopus)

Abstract

Background: Candida parapsilosis is a common cause of invasive candidiasis, especially in newborn infants, and infections have been increasing over the past two decades. C. parapsilosis has been primarily studied in pure culture, leaving gaps in understanding of its function in a microbiome context. Results: Here, we compare five unique C. parapsilosis genomes assembled from premature infant fecal samples, three of which are newly reconstructed, and analyze their genome structure, population diversity, and in situ activity relative to reference strains in pure culture. All five genomes contain hotspots of single nucleotide variants, some of which are shared by strains from multiple hospitals. A subset of environmental and hospital-derived genomes share variants within these hotspots suggesting derivation of that region from a common ancestor. Four of the newly reconstructed C. parapsilosis genomes have 4 to 16 copies of the gene RTA3, which encodes a lipid translocase and is implicated in antifungal resistance, potentially indicating adaptation to hospital antifungal use. Time course metatranscriptomics and metaproteomics on fecal samples from a premature infant with a C. parapsilosis blood infection revealed highly variable in situ expression patterns that are distinct from those of similar strains in pure cultures. For example, biofilm formation genes were relatively less expressed in situ, whereas genes linked to oxygen utilization were more highly expressed, indicative of growth in a relatively aerobic environment. In gut microbiome samples, C. parapsilosis co-existed with Enterococcus faecalis that shifted in relative abundance over time, accompanied by changes in bacterial and fungal gene expression and proteome composition. Conclusions: The results reveal potentially medically relevant differences in Candida function in gut vs. laboratory environments, and constrain evolutionary processes that could contribute to hospital strain persistence and transfer into premature infant microbiomes. [MediaObject not available: see fulltext.]

Original language	English
Article number	142
Number of pages	17
Journal	Microbiome
Volume	9
Issue number	1
DOIs	https://doi.org/10.1186/s40168-021-01085-y
Publication status	Published - 21 Jun 2021
Externally published	Yes

Keywords

Candida
Genome-resolved metagenomics
Hospital microbiome
Metagenomics
Microbial eukaryotes
Neonatal intensive care unit
Premature infants
Strain-tracking

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West, P. T., Peters, S. L., Olm, M. R., Yu, F. B., Gause, H., Lou, Y. C., Firek, B. A., Baker, R., Johnson, A. D., Morowitz, M. J., Hettich, R. L., & Banfield, J. F. (2021). Genetic and behavioral adaptation of Candida parapsilosis to the microbiome of hospitalized infants revealed by in situ genomics, transcriptomics, and proteomics. Microbiome, 9(1), Article 142. https://doi.org/10.1186/s40168-021-01085-y

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title = "Genetic and behavioral adaptation of Candida parapsilosis to the microbiome of hospitalized infants revealed by in situ genomics, transcriptomics, and proteomics",

abstract = "Background: Candida parapsilosis is a common cause of invasive candidiasis, especially in newborn infants, and infections have been increasing over the past two decades. C. parapsilosis has been primarily studied in pure culture, leaving gaps in understanding of its function in a microbiome context. Results: Here, we compare five unique C. parapsilosis genomes assembled from premature infant fecal samples, three of which are newly reconstructed, and analyze their genome structure, population diversity, and in situ activity relative to reference strains in pure culture. All five genomes contain hotspots of single nucleotide variants, some of which are shared by strains from multiple hospitals. A subset of environmental and hospital-derived genomes share variants within these hotspots suggesting derivation of that region from a common ancestor. Four of the newly reconstructed C. parapsilosis genomes have 4 to 16 copies of the gene RTA3, which encodes a lipid translocase and is implicated in antifungal resistance, potentially indicating adaptation to hospital antifungal use. Time course metatranscriptomics and metaproteomics on fecal samples from a premature infant with a C. parapsilosis blood infection revealed highly variable in situ expression patterns that are distinct from those of similar strains in pure cultures. For example, biofilm formation genes were relatively less expressed in situ, whereas genes linked to oxygen utilization were more highly expressed, indicative of growth in a relatively aerobic environment. In gut microbiome samples, C. parapsilosis co-existed with Enterococcus faecalis that shifted in relative abundance over time, accompanied by changes in bacterial and fungal gene expression and proteome composition. Conclusions: The results reveal potentially medically relevant differences in Candida function in gut vs. laboratory environments, and constrain evolutionary processes that could contribute to hospital strain persistence and transfer into premature infant microbiomes. [MediaObject not available: see fulltext.]",

keywords = "Candida, Genome-resolved metagenomics, Hospital microbiome, Metagenomics, Microbial eukaryotes, Neonatal intensive care unit, Premature infants, Strain-tracking",

author = "West, {Patrick T.} and Peters, {Samantha L.} and Olm, {Matthew R.} and Yu, {Feiqiao B.} and Haley Gause and Lou, {Yue Clare} and Firek, {Brian A.} and Robyn Baker and Johnson, {Alexander D.} and Morowitz, {Michael J.} and Hettich, {Robert L.} and Banfield, {Jillian F.}",

note = "Funding Information: This research was supported by the National Institutes of Health (NIH) under award RAI092531A, the Alfred P. Sloan Foundation under grant APSF-2012-10-05, and National Science Foundation Graduate Research Fellowships to P.W. under Grant No. DGE 1106400. This work used the Vincent J. Coates Genomics Sequencing Laboratory at UC Berkeley, supported by NIH S10 OD018174 Instrumentation Grant. Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = jun,

day = "21",

doi = "10.1186/s40168-021-01085-y",

language = "English",

volume = "9",

journal = "Microbiome",

issn = "2049-2618",

publisher = "BioMed Central",

number = "1",

}

West, PT, Peters, SL, Olm, MR, Yu, FB, Gause, H, Lou, YC, Firek, BA, Baker, R, Johnson, AD, Morowitz, MJ, Hettich, RL & Banfield, JF 2021, 'Genetic and behavioral adaptation of Candida parapsilosis to the microbiome of hospitalized infants revealed by in situ genomics, transcriptomics, and proteomics', Microbiome, vol. 9, no. 1, 142. https://doi.org/10.1186/s40168-021-01085-y

TY - JOUR

T1 - Genetic and behavioral adaptation of Candida parapsilosis to the microbiome of hospitalized infants revealed by in situ genomics, transcriptomics, and proteomics

AU - West, Patrick T.

AU - Peters, Samantha L.

AU - Olm, Matthew R.

AU - Yu, Feiqiao B.

AU - Gause, Haley

AU - Lou, Yue Clare

AU - Firek, Brian A.

AU - Baker, Robyn

AU - Johnson, Alexander D.

AU - Morowitz, Michael J.

AU - Hettich, Robert L.

AU - Banfield, Jillian F.

N1 - Funding Information: This research was supported by the National Institutes of Health (NIH) under award RAI092531A, the Alfred P. Sloan Foundation under grant APSF-2012-10-05, and National Science Foundation Graduate Research Fellowships to P.W. under Grant No. DGE 1106400. This work used the Vincent J. Coates Genomics Sequencing Laboratory at UC Berkeley, supported by NIH S10 OD018174 Instrumentation Grant. Publisher Copyright: © 2021, The Author(s).

PY - 2021/6/21

Y1 - 2021/6/21

N2 - Background: Candida parapsilosis is a common cause of invasive candidiasis, especially in newborn infants, and infections have been increasing over the past two decades. C. parapsilosis has been primarily studied in pure culture, leaving gaps in understanding of its function in a microbiome context. Results: Here, we compare five unique C. parapsilosis genomes assembled from premature infant fecal samples, three of which are newly reconstructed, and analyze their genome structure, population diversity, and in situ activity relative to reference strains in pure culture. All five genomes contain hotspots of single nucleotide variants, some of which are shared by strains from multiple hospitals. A subset of environmental and hospital-derived genomes share variants within these hotspots suggesting derivation of that region from a common ancestor. Four of the newly reconstructed C. parapsilosis genomes have 4 to 16 copies of the gene RTA3, which encodes a lipid translocase and is implicated in antifungal resistance, potentially indicating adaptation to hospital antifungal use. Time course metatranscriptomics and metaproteomics on fecal samples from a premature infant with a C. parapsilosis blood infection revealed highly variable in situ expression patterns that are distinct from those of similar strains in pure cultures. For example, biofilm formation genes were relatively less expressed in situ, whereas genes linked to oxygen utilization were more highly expressed, indicative of growth in a relatively aerobic environment. In gut microbiome samples, C. parapsilosis co-existed with Enterococcus faecalis that shifted in relative abundance over time, accompanied by changes in bacterial and fungal gene expression and proteome composition. Conclusions: The results reveal potentially medically relevant differences in Candida function in gut vs. laboratory environments, and constrain evolutionary processes that could contribute to hospital strain persistence and transfer into premature infant microbiomes. [MediaObject not available: see fulltext.]

AB - Background: Candida parapsilosis is a common cause of invasive candidiasis, especially in newborn infants, and infections have been increasing over the past two decades. C. parapsilosis has been primarily studied in pure culture, leaving gaps in understanding of its function in a microbiome context. Results: Here, we compare five unique C. parapsilosis genomes assembled from premature infant fecal samples, three of which are newly reconstructed, and analyze their genome structure, population diversity, and in situ activity relative to reference strains in pure culture. All five genomes contain hotspots of single nucleotide variants, some of which are shared by strains from multiple hospitals. A subset of environmental and hospital-derived genomes share variants within these hotspots suggesting derivation of that region from a common ancestor. Four of the newly reconstructed C. parapsilosis genomes have 4 to 16 copies of the gene RTA3, which encodes a lipid translocase and is implicated in antifungal resistance, potentially indicating adaptation to hospital antifungal use. Time course metatranscriptomics and metaproteomics on fecal samples from a premature infant with a C. parapsilosis blood infection revealed highly variable in situ expression patterns that are distinct from those of similar strains in pure cultures. For example, biofilm formation genes were relatively less expressed in situ, whereas genes linked to oxygen utilization were more highly expressed, indicative of growth in a relatively aerobic environment. In gut microbiome samples, C. parapsilosis co-existed with Enterococcus faecalis that shifted in relative abundance over time, accompanied by changes in bacterial and fungal gene expression and proteome composition. Conclusions: The results reveal potentially medically relevant differences in Candida function in gut vs. laboratory environments, and constrain evolutionary processes that could contribute to hospital strain persistence and transfer into premature infant microbiomes. [MediaObject not available: see fulltext.]

KW - Candida

KW - Genome-resolved metagenomics

KW - Hospital microbiome

KW - Metagenomics

KW - Microbial eukaryotes

KW - Neonatal intensive care unit

KW - Premature infants

KW - Strain-tracking

UR - http://www.scopus.com/inward/record.url?scp=85109037082&partnerID=8YFLogxK

U2 - 10.1186/s40168-021-01085-y

DO - 10.1186/s40168-021-01085-y

M3 - Article

C2 - 34154658

AN - SCOPUS:85109037082

SN - 2049-2618

VL - 9

JO - Microbiome

JF - Microbiome

IS - 1

M1 - 142

ER -

Genetic and behavioral adaptation of Candida parapsilosis to the microbiome of hospitalized infants revealed by in situ genomics, transcriptomics, and proteomics

Abstract

Keywords

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