Extensive genetic diversity, unique population structure and evidence of genetic exchange in the sexually transmitted parasite Trichomonas vaginalis

Background

Trichomonas vaginalis is the causative agent of human trichomoniasis, the most common non-viral sexually transmitted infection world-wide. Despite its prevalence, little is known about the genetic diversity and population structure of this haploid parasite due to the lack of appropriate tools. The development of a panel of microsatellite makers and SNPs from mining the parasite''s genome sequence has paved the way to a global analysis of the genetic structure of the pathogen and association with clinical phenotypes.

Methodology/Principal Findings

Here we utilize a panel of T. vaginalis-specific genetic markers to genotype 235 isolates from Mexico, Chile, India, Australia, Papua New Guinea, Italy, Africa and the United States, including 19 clinical isolates recently collected from 270 women attending New York City sexually transmitted disease clinics. Using population genetic analysis, we show that T. vaginalis is a genetically diverse parasite with a unique population structure consisting of two types present in equal proportions world-wide. Parasites belonging to the two types (type 1 and type 2) differ significantly in the rate at which they harbor the T. vaginalis virus, a dsRNA virus implicated in parasite pathogenesis, and in their sensitivity to the widely-used drug, metronidazole. We also uncover evidence of genetic exchange, indicating a sexual life-cycle of the parasite despite an absence of morphologically-distinct sexual stages.

Conclusions/Significance

Our study represents the first robust and comprehensive evaluation of global T. vaginalis genetic diversity and population structure. Our identification of a unique two-type structure, and the clinically relevant phenotypes associated with them, provides a new dimension for understanding T. vaginalis pathogenesis. In addition, our demonstration of the possibility of genetic exchange in the parasite has important implications for genetic research and control of the disease.     

Decreased premotor cortex volume in victims of urban violence with posttraumatic stress disorder

Background

Studies addressing posttraumatic stress disorder (PTSD) have demonstrated that PTSD patients exhibit structural abnormalities in brain regions that relate to stress regulation and fear responses, such as the hippocampus, amygdala, anterior cingulate cortex, and ventromedial prefrontal cortex. Premotor cortical areas are involved in preparing to respond to a threatening situation and in representing the peripersonal space. Urban violence is an important and pervasive cause of human suffering, especially in large urban centers in the developing world. Violent events, such as armed robbery, are very frequent in certain cities, and these episodes increase the risk of PTSD. Assaultive trauma is characterized by forceful invasion of the peripersonal space; therefore, could this traumatic event be associated with structural alteration of premotor areas in PTSD?

Methodology/Principal Findings

Structural magnetic resonance imaging scans were acquired from a sample of individuals that had been exposed to urban violence. This sample consisted of 16 PTSD patients and 16 age- and gender-matched controls. Psychometric questionnaires differentiated PTSD patients from trauma-exposed controls with regard to PTSD symptoms, affective, and resilience predispositions. Voxel-based morphometric analysis revealed that, compared with controls, the PTSD patients presented significant reductions in gray matter volume in the ventral premotor cortex and in the pregenual anterior cingulate cortex.

Conclusions

Volume reduction in the premotor cortex that is observed in victims of urban violence with PTSD may be associated with a disruption in the dynamical modulation of the safe space around the body. The finding that PTSD patients presented a smaller volume of pregenual anterior cingulate cortex is consistent with the results of other PTSD neuroimaging studies that investigated different types of traumatic events.     

Molecular cloning of structural and immunity genes for megacins A-216 and A-19213 in Bacillus megaterium.

A host-vector system was developed for molecular cloning in Bacillus megaterium and used to clone the structural and immunity genes for megacins A-216 and A-19213. Recombinant clones that expressed immunity only or both immunity to and production of each megacin were obtained. Restriction mapping of native megacinogenic plasmids and recombinant clones was used to construct physical and genetic maps of megacinogenic plasmids pBM309 and pBM113. Limited sequence homology between pBM309 and pBM113 was detected by Southern blot hybridization and was mapped to, at most, a 6.4-kilobase-pair region of pBM309 and a 6.1-kilobase-pair region of pBM113.     

Temporary sterility produced in male mice by 5-thio-D-glucose.

When 5-thio-D-glucose was fed to male mice at daily dose levels greater than 30 mg/kg sperm development was completely inhibited within 3 weeks and remained so without impairment of libido for the experimental period of 7 weeks. Removal of this substance from the diet resulted in a resumption of sperm development and fertility within 5 to 8 weeks. Normal litters were sired by males which had recovered after this treatment.     

ICAM-1-CD18 interaction mediates neutrophil cytotoxicity through protease release

Interaction ofthe ₂-integrin complex on thepolymorphonuclear neutrophil (PMN) with intercellular adhesionmolecule-1 (ICAM-1) has been implicated in PMN-mediated cytotoxicity.This study examined interaction of the CD11a, CD11b, and CD18 subunitsof the ₂-integrin with ICAM-1,transfected into Chinese hamster ovarian (CHO) cells to avoid effectsof other adhesion molecules. Incubation of quiescent PMNs withwild-type and ICAM-1-transfected CHO cells produced nominal cell lysis.Similarly, when phorbol myristate acetate (PMA)-activated PMNs wereincubated with wild-type CHO cells, minimal cytotoxicity was produced.However, when ICAM-1-transfected CHO cells were incubated withPMA-activated PMNs, 40% cell lysis occurred. Blockade with amonoclonal antibody (MAb) to ICAM-1 or MAbs to CD11a, CD11b, or CD18reduced PMN-mediated cytotoxicity to baseline. To examine the role ofadhesion in cytotoxicity, we studied₂-integrin-mediated PMNadhesion to ICAM-1-transfected CHO cells and found that MAbs for CD11a,CD11b, and CD18 all abrogated PMN cytotoxicity despite disparateeffects on adhesion. To assess the role of CD18,₂-integrin subunits werecross-linked, and CD18 alone mediated protease release. Moreover,ICAM-1 was immunoprecipitated from transfected CHO cells and incubatedwith PMNs. This soluble ICAM-1 provoked elastase release, similar toPMA, which could be inhibited by MAbs to CD18 but not MAbs to other₂-integrin subunits. Inaddition, coincubation with protease inhibitors eglin C and AAPVCKreduced PMN-mediated cytotoxicity to control levels. Finally,ICAM-1-transfected CHO cells were exposed to activated PMNs from apatient with chronic granulomatous disease that caused significant celllysis, equivalent to that of PMNs from normal donors. Collectively,these data suggest that ICAM-1 provokes PMN-mediated cytotoxicity viaCD18-mediated protease release.