Type VII secretion system and its effect on group B Streptococcus virulence in isolates obtained from newborns with early onset disease and colonized pregnant women

Yulia Schindler; Galia Rahav; Israel Nissan; Gal Valenci; Miriam Ravins; Emanuel Hanski; Dana Ment; Dorit Tekes-Manova; Yasmin Maor

doi:10.3389/fcimb.2023.1168530

Type VII secretion system and its effect on group B Streptococcus virulence in isolates obtained from newborns with early onset disease and colonized pregnant women

Front Cell Infect Microbiol. 2023 Jul 21:13:1168530. doi: 10.3389/fcimb.2023.1168530. eCollection 2023.

Authors

Yulia Schindler^{1

2}, Galia Rahav^{2

3}, Israel Nissan^{3

4}, Gal Valenci⁴, Miriam Ravins⁵, Emanuel Hanski⁵, Dana Ment⁶, Dorit Tekes-Manova¹, Yasmin Maor^{2

7}

Affiliations

¹ Microbiology Laboratory, Mayanei Hayeshua Medical Center, Bney Brak, Israel.
² The Sackler School of Medicine, Tel Aviv University, Tel Aviv, Israel.
³ Infectious Disease Unit, Sheba Medical Center, Ramat-Gan, Israel.
⁴ National Public Health Laboratory, Ministry of Health (Israel), Tel-Aviv, Israel.
⁵ Department of Microbiology and Molecular Genetics, The Institute for Medical Research, Israel-Canada (IMRIC), Faculty of Medicine, Jerusalem, Israel.
⁶ Department of Plant Pathology and Weed Research, Plant Protection Institute, Agricultural Research Organization, Volcani Institute, Rishon LeZion, Israel.
⁷ Infectious Disease Unit, Wolfson Medical Center, Holon, Israel.

Abstract

Introduction: GBS may cause a devastating disease in newborns. In early onset disease of the newborn the bacteria are acquired from the colonized mother during delivery. We characterized type VII secretion system (T7SS), exporting small proteins of the WXG100 superfamily, in group B Streptococci (GBS) isolates from pregnant colonized women and newborns with early onset disease (EOD) to better understand T7SS contribution to virulence in these different clinical scenarios.

Methods: GBS genomes [N=33, 17 EOD isolates (serotype III/ST17) and 16 colonizing isolates (12 serotype VI/ST1, one serotype VI/ST19, one serotype VI/ST6, and two serotype 3/ST19)] were analyzed for presence of T7SS genes and genes encoding WXG100 proteins. We also perform bioinformatic analysis. Galleria mellonella larvae were used to compare virulence between colonizing, EOD, and mutant EOD isolates. The EOD isolate number 118659 (III/ST17) was used for knocking out the essC gene encoding a membrane-bound ATPase, considered the driver of T7SS.

Results: Most GBS T7SS loci encoded core component genes: essC, membrane-embedded proteins (essA; essB), modulators of T7SS activity (esaA; esaB; esaC) and effectors: [esxA (SAG1039); esxB (SAG1030)].Bioinformatic analysis indicated that based on sequence type (ST) the clinicalGBS isolates encode at least three distinct subtypes of T7SS machinery. In all ST1isolates we identified two copies of esxA gene (encoding putative WXG100proteins), when only 23.5% of the ST17 isolates harbored the esxA gene. Five ST17isolates encoded two copies of the essC gene. Orphaned WXG100 molecule(SAG0230), distinct from T7SS locus, were found in all tested strains, except inST17 strains where the locus was found in only 23.5% of the isolates. In ST6 andST19 isolates most of the structure T7SS genes were missing. EOD isolates demonstrated enhanced virulence in G. mellonella modelcompared to colonizing isolates. The 118659DessC strain was attenuated in itskilling ability, and the larvae were more effective in eradicating 118659DessC.

Conclusions: We demonstrated that T7SS plays a role during infection. Knocking out the essC gene, considered the driver of T7SS, decreased the virulence of ST17 responsible for EOD, causing them to be less virulent comparable to the virulence observed in colonizing isolates.

Keywords: Streptococcus agalactiae; early onset disease; neonate; pregnancy; sepsis; type 7 secretion system; virulence.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Female
Humans
Infant, Newborn
Membrane Proteins / genetics
Pregnancy
Pregnant Women
Serogroup
Streptococcal Infections* / microbiology
Streptococcus agalactiae / genetics
Type VII Secretion Systems* / genetics
Type VII Secretion Systems* / metabolism
Virulence / genetics

Substances

Type VII Secretion Systems
Membrane Proteins

Grants and funding

The study was funded by internal funds of the Microbiology laboratory, Mayaney Hayeshua, Bney Brak, Israel and the Infectious Disease Unit, Sheba Medical Center.