HtpS, a novel immunogenic cell surface-exposed protein of Streptococcus suis, confers protection in mice

Shao, Zhu‐Qing; Pan, Xiuzhen; Li, Xianfu; Liu, Wenjing; Han, MeiLan K.; Wang, Changjun; Wang, Jing; Feng, Zijian; Cao, Min; Tang, Jiaqi

doi:10.1111/j.1574-6968.2010.02162.x

Cited by 31 publications

(26 citation statements)

References 36 publications

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“…In addition to six previously identified elements (capsular polysaccharides [CPS], 20 , 101 extracellular protein factor [EF], 102 fibronectin binding factor [FBP], 103 muramidase-released protein [MRP], 102 a protein of 38 kDa localized on bacterial surface [abbreviated 38 kDa], 104 and thio-activated hemolysin with known crystal structure [Suilysin, SLY]) 105 , 106 plus implication into bacterial meningitis, 107 11 more members have been supplemented into this group that include SspA, the surface-associated subtilisin-like serine protease, 41 , 108 , 109 HtpS, a novel immunogenic cell surface-exposed protein, 110 and Sat surface protein 111 , 112 (Table 2). Like FBP, 103 the gene SSU05_1311 with unknown function was determined to be one more surface anchored fibronectin-binding protein.…”

Section: Molecular Mechanism For Streptococcus Suis Infectionmentioning

confidence: 99%

“…In addition, HtpS, a putative member of histidine triad protein family, was determined to be cell surface-associated protein that was expressed during the infection of Chinese SS2 strain 05ZYH33 110 . Moreover, recombinant HtpS protein was demonstrated to function as a protective antigen against SS2 infections 110 . Similarly, Zhang et al 124 recently defined another new infection-associated antigen protein, Trag, using in vivo-induced antigen technology (IVIAT).…”

Section: Molecular Mechanism For Streptococcus Suis Infectionmentioning

confidence: 99%

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Streptococcus suisinfection

et al. 2014

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Streptococcus suis (S. suis) is a family of pathogenic gram-positive bacterial strains that represents a primary health problem in the swine industry worldwide. S. suis is also an emerging zoonotic pathogen that causes severe human infections clinically featuring with varied diseases/syndromes (such as meningitis, septicemia, and arthritis). Over the past few decades, continued efforts have made significant progress toward better understanding this zoonotic infectious entity, contributing in part to the elucidation of the molecular mechanism underlying its high pathogenicity. This review is aimed at presenting an updated overview of this pathogen from the perspective of molecular epidemiology, clinical diagnosis and typing, virulence mechanism, and protective antigens contributing to its zoonosis.

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Section: Molecular Mechanism For Streptococcus Suis Infectionmentioning

confidence: 99%

Section: Molecular Mechanism For Streptococcus Suis Infectionmentioning

confidence: 99%

Streptococcus suisinfection

et al. 2014

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“…Even though their individual physiological functions are not yet fully understood, their highly immunogenic character defines them as potential vaccine antigens [33], [34]. Indeed, administration of PhtA, PhtE or PhtD (also referred to as HtpS in Streptococcus suis ) protects mice against S. pneumoniae colonization of the nasopharynx and against bacteremia by inducing a humoral response [35], [36], [37]. In this context, PhtD appears especially attractive because it shows the uppermost efficacy of protection in nasopharyngeal colonization models and displays the highest level of conservation among S. pyogenes , S. agalactiae , S. suis and S. pneumoniae [37], [38], [39] as well as across pneumococcal serotypes [40], [41].…”

Section: Introductionmentioning

confidence: 99%

“…Indeed, administration of PhtA, PhtE or PhtD (also referred to as HtpS in Streptococcus suis ) protects mice against S. pneumoniae colonization of the nasopharynx and against bacteremia by inducing a humoral response [35], [36], [37]. In this context, PhtD appears especially attractive because it shows the uppermost efficacy of protection in nasopharyngeal colonization models and displays the highest level of conservation among S. pyogenes , S. agalactiae , S. suis and S. pneumoniae [37], [38], [39] as well as across pneumococcal serotypes [40], [41]. In addition, single phtD deletion in S. pneumoniae induces significant attenuation in intranasal challenge model [25] suggesting its involvement in the pathogenesis of pneumococcal diseases.…”

Section: Introductionmentioning

confidence: 99%

New Insights into Histidine Triad Proteins: Solution Structure of a Streptococcus pneumoniae PhtD Domain and Zinc Transfer to AdcAII

et al. 2013

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Zinc (Zn2+) homeostasis is critical for pathogen host colonization and invasion. Polyhistidine triad (Pht) proteins, located at the surface of various streptococci, have been proposed to be involved in Zn2+ homeostasis. The phtD gene, coding for a Zn2+-binding protein, is organized in an operon with adcAII coding for the extracellular part of a Zn2+ transporter. In the present work, we investigate the relationship between PhtD and AdcAII using biochemical and structural biology approaches. Immuno-precipitation experiments on purified membranes of Streptococcus pneumoniae (S. pneumoniae) demonstrate that native PhtD and AdcAII interact in vivo confirming our previous in vitro observations. NMR was used to demonstrate Zn2+ transfer from the Zn2+-bound form of a 137 amino acid N-terminal domain of PhtD (t-PhtD) to AdcAII. The high resolution NMR structure of t-PhtD shows that Zn2+ is bound in a tetrahedral site by histidines 83, 86, and 88 as well as by glutamate 63. Comparison of the NMR parameters measured for apo- and Zn2+-t-PhtD shows that the loss of Zn2+ leads to a diminished helical propensity at the C-terminus and increases the local dynamics and overall molecular volume. Structural comparison with the crystal structure of a 55-long fragment of PhtA suggests that Pht proteins are built from short repetitive units formed by three β-strands containing the conserved HxxHxH motif. Taken together, these results support a role for S. pneumoniae PhtD as a Zn2+ scavenger for later release to the surface transporter AdcAII, leading to Zn2+ uptake.

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“…Adamou et al [19] found that although the sequence identity among four pht genes in S. pneumoniae varied from only 32% to 87%, a typical character of 4–6 duplicated histidine triad motifs was consistently shared by each protein. Searching for this signature, researchers subsequently identified genes homologous to pht genes in two other human pathogens, S. pyogenes [18], [22] and S. agalactiae [23]; and also in the zoonotic pathogen S. suis [24], [25]. The identified pht homologs were named, htp A and slr in S. pyogenes ; sht and blr in S. agalactiae ; and htpS in S. suis .…”

Section: Introductionmentioning

confidence: 99%

Insight into the Evolution of the Histidine Triad Protein (HTP) Family in Streptococcus

et al. 2013

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The Histidine Triad Proteins (HTPs), also known as Pht proteins in Streptococcus pneumoniae, constitute a family of surface-exposed proteins that exist in many pathogenic streptococcal species. Although many studies have revealed the importance of HTPs in streptococcal physiology and pathogenicity, little is known about their origin and evolution. In this study, after identifying all htp homologs from 105 streptococcal genomes representing 38 different species/subspecies, we analyzed their domain structures, positions in genome, and most importantly, their evolutionary histories. By further projecting this information onto the streptococcal phylogeny, we made several major findings. First, htp genes originated earlier than the Streptococcus genus and gene-loss events have occurred among three streptococcal groups, resulting in the absence of the htp gene in the Bovis, Mutans and Salivarius groups. Second, the copy number of htp genes in other groups of Streptococcus is variable, ranging from one to four functional copies. Third, both phylogenetic evidence and domain structure analyses support the division of two htp subfamilies, designated as htp I and htp II. Although present mainly in the pyogenic group and in Streptococcus suis, htp II members are distinct from htp I due to the presence of an additional leucine-rich-repeat domain at the C-terminus. Finally, htp genes exhibit a faster nucleotide substitution rate than do housekeeping genes. Specifically, the regions outside the HTP domains are under strong positive selection. This distinct evolutionary pattern likely helped Streptococcus to easily escape from recognition by host immunity.

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HtpS, a novel immunogenic cell surface-exposed protein of Streptococcus suis, confers protection in mice

Cited by 31 publications

References 36 publications

Streptococcus suisinfection

Streptococcus suisinfection

New Insights into Histidine Triad Proteins: Solution Structure of a Streptococcus pneumoniae PhtD Domain and Zinc Transfer to AdcAII

Insight into the Evolution of the Histidine Triad Protein (HTP) Family in Streptococcus

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