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Cyclization increases bactericidal activity of arginine-rich cationic cell-penetrating peptide for Neisseria gonorrhoeae
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ABSTRACT
We previously reported that a linear cationic 12-amino acid cell-penetrating peptide (CPP) was bactericidal for
Neisseria gonorrhoeae
. In this study, our objectives were to determine the effect of cyclization of the linear CPP on its antibacterial activity for
N. gonorrhoeae
and cytotoxicity for human cells. We compared the bactericidal effect of 4-hour treatment with the linear CPP to that of CPPs cyclized by a thioether or a disulfide bond on human challenge and multi-drug resistant (MDR) strains of
N. gonorrhoeae
grown in cell culture media with 10% fetal bovine serum (FBS). The effect of lipooligosaccharide (LOS) sialylation on bactericidal activity was analyzed. We determined the ability of the CPPs to treat human cells infected
in vitro
with
N. gonorrhoeae
, to reduce the inflammatory response of human monocytic cells to gonococci, to kill strains of three commensal
Neisseria
species, and to inhibit gonococcal biofilms. The cyclized CPPs killed 100% of gonococci from all strains at 100 µM and >90% at 20 µM and were more potent than the linear form. The thioether-linked but not the disulfide-linked CPP was less cytotoxic for human cervical cells compared to the linear CPP. LOS sialylation had minimal effect on bactericidal activity. In treating infected human cells, the thioether-linked CPP at 20 µM killed >60% of extra- and intracellular bacteria and reduced TNF-α expression by THP-1 cells. The potency of the CPPs for the pathogenic and the commensal
Neisseria
was similar. The thioether-linked CPP partially eradicated gonococcal biofilms. Future studies will focus on determining efficacy in the female mouse model of gonorrhea.
IMPORTANCE
Neisseria gonorrhoeae
remains a major cause of sexually transmitted infections with 82 million cases worldwide in 2020, and 710,151 confirmed cases in the US in 2021, up 25% from 2017.
N. gonorrhoeae
can infect multiple tissues including the urethra, cervix, rectum, pharynx, and conjunctiva. The most serious sequelae are suffered by infected women as gonococci ascend to the upper reproductive tract and cause pelvic inflammatory disease, chronic pelvic pain, and infertility in 10%–20% of women. Control of gonococcal infection is widely recognized as increasingly challenging due to the lack of any vaccine.
N. gonorrhoeae
has quickly developed resistance to all but one class of antibiotics and the emergence of multidrug-resistant strains could result in untreatable infections. As such, gonorrhea is classified by the Center for Disease Control (CDC) as an urgent public health threat. The research presented herein on new therapeutics for gonorrhea has identified a cyclic cell-penetrating peptide (CPP) as a potent molecule targeting
N. gonorrhoeae
.
American Society for Microbiology
Title: Cyclization increases bactericidal activity of arginine-rich cationic cell-penetrating peptide for
Neisseria gonorrhoeae
Description:
ABSTRACT
We previously reported that a linear cationic 12-amino acid cell-penetrating peptide (CPP) was bactericidal for
Neisseria gonorrhoeae
.
In this study, our objectives were to determine the effect of cyclization of the linear CPP on its antibacterial activity for
N.
gonorrhoeae
and cytotoxicity for human cells.
We compared the bactericidal effect of 4-hour treatment with the linear CPP to that of CPPs cyclized by a thioether or a disulfide bond on human challenge and multi-drug resistant (MDR) strains of
N.
gonorrhoeae
grown in cell culture media with 10% fetal bovine serum (FBS).
The effect of lipooligosaccharide (LOS) sialylation on bactericidal activity was analyzed.
We determined the ability of the CPPs to treat human cells infected
in vitro
with
N.
gonorrhoeae
, to reduce the inflammatory response of human monocytic cells to gonococci, to kill strains of three commensal
Neisseria
species, and to inhibit gonococcal biofilms.
The cyclized CPPs killed 100% of gonococci from all strains at 100 µM and >90% at 20 µM and were more potent than the linear form.
The thioether-linked but not the disulfide-linked CPP was less cytotoxic for human cervical cells compared to the linear CPP.
LOS sialylation had minimal effect on bactericidal activity.
In treating infected human cells, the thioether-linked CPP at 20 µM killed >60% of extra- and intracellular bacteria and reduced TNF-α expression by THP-1 cells.
The potency of the CPPs for the pathogenic and the commensal
Neisseria
was similar.
The thioether-linked CPP partially eradicated gonococcal biofilms.
Future studies will focus on determining efficacy in the female mouse model of gonorrhea.
IMPORTANCE
Neisseria gonorrhoeae
remains a major cause of sexually transmitted infections with 82 million cases worldwide in 2020, and 710,151 confirmed cases in the US in 2021, up 25% from 2017.
N.
gonorrhoeae
can infect multiple tissues including the urethra, cervix, rectum, pharynx, and conjunctiva.
The most serious sequelae are suffered by infected women as gonococci ascend to the upper reproductive tract and cause pelvic inflammatory disease, chronic pelvic pain, and infertility in 10%–20% of women.
Control of gonococcal infection is widely recognized as increasingly challenging due to the lack of any vaccine.
N.
gonorrhoeae
has quickly developed resistance to all but one class of antibiotics and the emergence of multidrug-resistant strains could result in untreatable infections.
As such, gonorrhea is classified by the Center for Disease Control (CDC) as an urgent public health threat.
The research presented herein on new therapeutics for gonorrhea has identified a cyclic cell-penetrating peptide (CPP) as a potent molecule targeting
N.
gonorrhoeae
.
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