Oxamniquine resistance alleles are widespread in Old World Schistosoma mansoni and predate drug deployment

Chevalier, Frédéric D.; Clec’h, Winka Le; McDew-White, Marina; Menon, Vinay; Guzman, Meghan A.; Holloway, S.; Cao, Xiaoguang; Taylor, Alexander B.; Kinung’hi, Safari; Gouvras, Anouk N.; Webster, Bonnie L.; Webster, Joanne P.; Emery, Aidan M.; Rollinson, David; Djirmay, Amadou Garba; Mashikhi, Khalid M. Al; Yafae, Salem Al; Idris, Mohamed A.; Moné, Hélène; Mouahid, Gabriel; Hart, P. John; LoVerde, Philip T.; Anderson, Timothy J.

doi:10.1371/journal.ppat.1007881

Cited by 29 publications

(31 citation statements)

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“…The phenotypic and genetic data from this setting suggest that natural variation in this schistosome population has some praziquantel resistance or tolerance (we could not differentiate these with our data). This is consistent with evidence of natural variation in resistance within schistosomes predating drug use to a former anti-schistosomal drug, oxaminiquine, where resistance alleles are known [58].…”

Section: Discussionsupporting

confidence: 83%

Two-year longitudinal survey reveals high genetic diversity of Schistosoma mansoni with adult worms surviving praziquantel treatment at the start of mass drug administration in Uganda

et al. 2019

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BackgroundA key component of schistosomiasis control is mass drug administration with praziquantel. While control interventions have been successful in several endemic regions, mass drug administration has been less effective in others. Here we focus on the impact of repeated praziquantel treatment on the population structure and genetic diversity of Schistosoma mansoni.MethodsWe examined S. mansoni epidemiology, population genetics, and variation in praziquantel susceptibility in parasites isolated from children across three primary schools in a high endemicity region at the onset of the Ugandan National Control Programme. Children were sampled at 11 timepoints over two years, including one week and four weeks post-praziquantel treatment to evaluate short-term impacts on clearance and evidence of natural variation in susceptibility to praziquantel.ResultsPrevalence of S. mansoni was 85% at baseline. A total of 3576 miracidia larval parasites, isolated from 203 individual children, were genotyped at seven loci. Overall, genetic diversity was high and there was low genetic differentiation, indicating high rates of parasite gene flow. Schistosome siblings were found both pre-treatment and four weeks post-treatment, demonstrating adult worms surviving treatment and natural praziquantel susceptibility variation in these populations at the beginning of mass drug administration. However, we did not find evidence for selection on these parasites. While genetic diversity decreased in the short-term (four weeks post-treatment), diversity did not decrease over the entire period despite four rounds of mass treatment. Furthermore, within-host genetic diversity was affected by host age, host sex, infection intensity and recent praziquantel treatment.ConclusionsOur findings suggest that praziquantel treatments have short-term impacts on these parasite populations but impacts were transient and no long-term reduction in genetic diversity was observed. High gene flow reduces the likelihood of local adaptation, so even though parasites surviving treatment were observed, these were likely to be diluted at the beginning of the Ugandan National Control Programme. Together, these results suggest that MDA in isolation may be insufficient to reduce schistosome populations in regions with high genetic diversity and gene flow.

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Section: Discussionsupporting

confidence: 83%

Two-year longitudinal survey reveals high genetic diversity of Schistosoma mansoni with adult worms surviving praziquantel treatment at the start of mass drug administration in Uganda

et al. 2019

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“…None of these SNPs affect Ca 2+ influx: they are therefore unlikely to have determined critical residues that determine binding between PZQ and Sm.TRPMPZQ (21). We examined the mutations present in Sm.TRPMPZQ in natural schistosome populations using exome sequencing from 259 miracidia, cercariae or adult parasites from 3 African countries (Senegal, Niger, Tanzania), the Middle East (Oman) and South America (Brazil) (51,52). We were able to sequence 36/41 exons of Sm.TRPMPZQ from 122/259 parasites on average (s.e.…”

Section: Chemical Blockers and Activators Of Smtrpmpzq Modulate Pzq-rmentioning

confidence: 99%

Genetic analysis of praziquantel response in schistosome parasites implicates a transient receptor potential channel

et al. 2021

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Mass treatment with praziquantel (PZQ) monotherapy is the mainstay for schistosome treatment. This drug shows imperfect cure rates in the field and parasites showing reduced response to PZQ can be selected in the laboratory, but the extent of resistance in Schistosoma mansoni populations is unknown. We examined the genetic basis of variation in PZQ response in a S. mansoni population (SmLE-PZQ-R) selected with PZQ in the laboratory: 35% of these worms survive high dose (73 µg/mL) PZQ treatment. We used genome wide association to map loci underlying PZQ response. The major chr. 3 peak shows recessive inheritance and contains a transient receptor potential (Sm.TRPMPZQ) channel (Smp_246790), activated by nanomoles of PZQ. Marker-assisted selection of parasites at a single Sm.TRPMPZQ SNP enriched populations of PZQ-R and PZQ-S parasites showing >377 fold difference in PZQ response. The PZQ-R parasites survived treatment in rodents better than PZQ-S. Resistant parasites show 2.25-fold lower expression of Sm.TRPMPZQ than sensitive parasites. Specific chemical blockers of Sm.TRPMPZQ enhanced PZQ resistance, while Sm.TRPMPZQ activators increased sensitivity. A single SNP in Sm.TRPMPZQ differentiated PZQ-ER and PZQ-ES lines, but mutagenesis showed this was not involved in PZQ-R, suggesting linked regulatory changes. We surveyed Sm.TRPMPZQ sequence variation in 259 individual parasites from the Newand Old World revealing one nonsense mutation, that results in a truncated protein with no PZQ binding site. Our results demonstrate that Sm.TRPMPZQ underlies variation in PZQ response in S. mansoni and provides an approach for monitoring emerging PZQ-resistance alleles in schistosome elimination programs..

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“…These findings also suggested that resistance to PZQ may be unlikely to establish or spread in these populations at the beginning of the national control program, given the current selection of targeting school-aged children alone. 69 Nevertheless, these studies on S. mansoni susceptibility to PZQ (at least within Uganda), as recent findings have shown for oxamniquine resistance, 66 have identified standing variation in drug efficacies and clearance rates on which selection can act. This might indeed be expected to accentuate as drug pressures over time increase.…”

Section: Introductionmentioning

confidence: 99%

“…The rate and likelihood of resistance developing is influenced by a broad range of factors including, but not exclusive to, baseline parasite genetic structure and underlying standing variation in drug tolerance on which selection can act, effective population size, refugia, and gene flow in parallel to treatment frequency, dosage, and whether single or combination drug regimens. 66 , 67 Figure 4 demonstrates how population genetics can, nevertheless, help evaluate and contribute to the detection of potential changes in drug resistance efficacy.…”

Section: Introductionmentioning

confidence: 99%

Parasite Population Genetic Contributions to the Schistosomiasis Consortium for Operational Research and Evaluation within Sub-Saharan Africa

Webster

Neves

Webster

et al. 2020

The American Journal of Tropical Medicine and Hygiene

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. Analyses of the population genetic structure of schistosomes under the “Schistosomiasis Consortium for Operational Research and Evaluation” (SCORE) contrasting treatment pressure scenarios in Tanzania, Niger, and Zanzibar were performed to provide supplementary critical information with which to evaluate the impact of these large-scale control activities and guide how activities could be adjusted. We predicted that population genetic analyses would reveal information on a range of important parameters including, but not exclusive to, recruitment and transmission of genotypes, occurrence of hybridization events, differences in reproductive mode, and degrees of inbreeding, and hence, the evolutionary potential, and responses of parasite populations under contrasting treatment pressures. Key findings revealed that naturally high levels of gene flow and mixing of the parasite populations between neighboring sites were likely to dilute any effects imposed by the SCORE treatment arms. Furthermore, significant inherent differences in parasite fecundity were observed, independent of current treatment arm, but potentially of major impact in terms of maintaining high levels of ongoing transmission in persistent “biological hotspot” sites. Within Niger, naturally occurring Schistosoma haematobium/Schistosoma bovis viable hybrids were found to be abundant, often occurring in significantly higher proportions than that of single-species S. haematobium infections. By examining parasite population genetic structures across hosts, treatment regimens, and the spatial landscape, our results to date illustrate key transmission processes over and above that which could be achieved through standard parasitological monitoring of prevalence and intensity alone, as well as adding to our understanding of Schistosoma spp. life history strategies in general.

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Oxamniquine resistance alleles are widespread in Old World Schistosoma mansoni and predate drug deployment

Cited by 29 publications

References 69 publications

Two-year longitudinal survey reveals high genetic diversity of Schistosoma mansoni with adult worms surviving praziquantel treatment at the start of mass drug administration in Uganda

Two-year longitudinal survey reveals high genetic diversity of Schistosoma mansoni with adult worms surviving praziquantel treatment at the start of mass drug administration in Uganda

Genetic analysis of praziquantel response in schistosome parasites implicates a transient receptor potential channel

Parasite Population Genetic Contributions to the Schistosomiasis Consortium for Operational Research and Evaluation within Sub-Saharan Africa

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