Evidence Against Rapid Emergence of Praziquantel Resistance in Schistosoma haematobium, Kenya.We examined the long-term efficacy of praziquantel praziquantel /pra·zi·quan·tel/ (pra?zi-kwahn´t'l) a broad-spectrum anthelmintic used for the treatment of a wide variety of fluke and tapeworm infections. pra·zi·quan·tel n. against Schistosoma haematobium Schistosoma hae·ma·to·bi·um n. A parasitic trematode found in the portal system, bladder, and rectum and common throughout Africa and parts of the Middle East. It causes schistosomiasis haematobium. , the causative agent of urinary schistosomiasis schistosomiasis (shĭs`təsōmī`əsĭs), bilharziasis, or snail fever, parasitic disease caused by blood flukes, trematode worms of the genus Schistosoma. , during a school-based treatment program in the Msambweni area of Coast Province, Kenya, where the disease is highly endemic. Our results, derived from treating 4,031 of 7,641 children from 1984 to 1993, indicate substantial year-to-year variation in drug efficacy. However, the pattern of this variation was not consistent with primary or progressive emergence of praziquantel resistance. Mathematical modeling indicated that, at current treatment rates, praziquantel resistance will likely take 10 or more years to emerge. Schistosomiasis remains a public health problem in many regions, including Africa, the Middle East, Asia, and South America South America, fourth largest continent (1991 est. pop. 299,150,000), c.6,880,000 sq mi (17,819,000 sq km), the southern of the two continents of the Western Hemisphere. (1). For many of the Schistosoma species that infect humans, isoquinolin-4-one, praziquantel, is the only effective drug (2,3). Its minimal side effects Side effects Effects of a proposed project on other parts of the firm. and high degree of efficacy against both trematodes and cestodes have made it the drug of choice for many human and veterinary parasitic infections (2,4). However, praziquantel has been in use for more than 20 years (5), and concern is increasing that resistance has emerged, or will soon emerge, in human parasites (6,7). Loss of praziquantel efficacy would set back helminth helminth /hel·minth/ (hel´minth) a parasitic worm. hel·minth n. A worm, especially a parasitic roundworm or tapeworm. Helminth A type of parasitic worm. control efforts. Many community-based programs depend on praziquantel for treating patients with schistosomiasis, cysticercosis cysticercosis /cys·ti·cer·co·sis/ (sis?ti-ser-ko´sis) infection with cysticerci. In humans, infection with the larval forms of Taenia solium. cys·ti·cer·co·sis n. , echinococcosis Echinococcosis Definition Echinococcosis (Hydatid disease) refers to human infection by the immature (larval) form of tapeworm, Echinococcus. One of three forms of the Echinococcus spp., E. , and tapeworm tapeworm, name for the parasitic flatworms forming the class Cestoda. All tapeworms spend the adult phase of their lives as parasites in the gut of a vertebrate animal (called the primary host). and other fluke infections Fluke Infections Definition Fluke infections are diseases of the digestive tract and other organ systems caused by several different species of parasitic flatworms (Trematodes) that have complex life cycles involving hosts other than human beings. (5,8-13). Concern over possible loss of efficacy prompted the European Commission European Commission, branch of the governing body of the European Union (EU) invested with executive and some legislative powers. Located in Brussels, Belgium, it was founded in 1967 when the three treaty organizations comprising what was then the European Community to establish an International Initiative on Praziquantel Use, which met in February 1998 (14) and again in February 1999 (15). The group reviewed reports of low efficacy in clinical trials in Senegal and Egypt (16-19) and of laboratory isolation of schistosome schistosome /schis·to·some/ (shis´-) (skis´to-som) an individual of the genus Schistosoma. schis·to·some n. strains resistant to standard and high doses of the drug (20-23). Although there was no definitive laboratory evidence of genetically transmissible transmissible /trans·mis·si·ble/ (trans-mis´i-b'l) capable of being transmitted. trans·mis·si·ble adj. Capable of being conveyed from one person to another. and drug-selectable resistance (as had been demonstrated for the antischistosome drug hycanthone [24]), concern was raised over possible low-level resistance. The need was expressed for continued monitoring for resistant strains under the pressure of widespread praziquantel use (14). We examined drug efficacy in the community and among schoolchildren schoolchildren school npl → écoliers mpl; (at secondary school) → collégiens mpl; lycéens mpl schoolchildren school given repeated praziquantel treatment for S. haematobium in Coast Province, Kenya. Year-to-year variation in treatment response was assessed, and the likely time-to-emergence of resistance was evaluated through the use of mathematical modeling of resistance-gene transmission in this obligately diecious diecious /di·e·cious/ (di-e´shus) sexually distinct; denoting species in which male and female genitals do not occur in the same individual. di·e·cious adj. Variant of dioecious. parasite. Materials and Methods Study Design The overall goal of the community study was to treat urinary schistosomiasis in schoolchildren (initial N - 3,196) in a nine-village area in Kwale District Kwale District is an administrative district in the Coast Province of Kenya. Its capital town is Kwale, although Msabweni and Ukunda are larger. The district has a population of 496.133 [1]. , Coast Province, Kenya. After oral informed consent was obtained under a human investigations protocol approved by the institutional review boards of University Hospitals of Cleveland University Hospitals is a major not-for-profit medical center in Cleveland, Ohio, United States. With 150 locations throughout northeast Ohio, it encompasses a network of hospitals, outpatient centers and primary care physicians. and the Ministry of Health, Kenya, case-finding was performed by school-based and follow-up village surveys. Details of the protocols have been published (25-27). In 1984, the initial treatment year, S. haematobium-infected children were randomly assigned to groups for treatment with either praziquantel (Biltricide, Bayer, Leverkusen, Germany), 40 mg/kg once a year, or metrifonate (Bilarcil, Bayer), 10 mg/kg three times a year. In years 2 and 3, the initial treatment was repeated, independent of parasitologic findings. New entrants to the study were assigned randomly to either the praziquantel or metrifonate treatment groups, according to according to prep. 1. As stated or indicated by; on the authority of: according to historians. 2. In keeping with: according to instructions. 3. the original 1984 protocol. In 1987, half the 1984 cohort, treated either with praziquantel or with metrifonate, was randomized ran·dom·ize tr.v. ran·dom·ized, ran·dom·iz·ing, ran·dom·iz·es To make random in arrangement, especially in order to control the variables in an experiment. to receive a single dose of metrifonate, 10 mg/kg, as a "consolidation" treatment. After a 2-year hiatus, annual treatment was resumed in 1989 to 1991; during this period, only children in whose urine samples eggs were identified (egg-positive children) were treated with praziquantel alone. Infection status was determined by Nuclepore (Whatman, Kent, UK) filtration of two 10-mL samples from stirred midday urine specimens. Infection-associated disease was determined by physical examination, dipstick dipstick /dip·stick/ (dip´stik) a strip of cellulose chemically impregnated to render it sensitive to protein, glucose, or other substances in the urine. urine examination for hematuria hematuria Blood in the urine. It usually indicates injury or disease of the kidney or another structure of the urinary system or possibly, in males, the reproductive system. It may result from infection, inflammation, tumours, kidney stones, or other disorders. and proteinuria proteinuria /pro·tein·uria/ (-ur´e-ah) an excess of serum proteins in the urine, as in renal disease or after strenuous exercise.proteinu´ric pro·tein·u·ri·a n. 1. , and ultrasound examination Ultrasound examination A medical test in which high frequency sound waves are directed at a particular internal area of the body. As the sound waves are reflected by internal structures, a computer uses the data to construct an image of the structures. of the kidneys and bladder (25). Clinical and parasitologic testing was performed each year. Results were coded and entered for analysis in databases at Case Western Reserve University and the Kenyan Ministry of Health. Data Analysis Results of annual treatments were scored as "cure" for patients whose status changed from egg-positive to egg-negative, "noncure" for those whose status remained egg-positive, and "infected or reinfected" for those whose status changed from egg-negative to egg-positive between yearly examinations. Because of the skewed distribution Skewed distribution Probability distribution in which an unequal number of observations lie below (negative skew) or above (positive skew) the mean. of egg counts in the infected population, the effects of treatment on average intensity of infection were assessed by determining the change in geometric mean (mathematics) geometric mean - The Nth root of the product of N numbers. If each number in a list of numbers was replaced with their geometric mean, then multiplying them all together would still give the same result. egg count between examinations. Differences between outcome rates were assessed by the chi-square test chi-square test: see statistics. with Yates' correction or Fisher's exact test Fisher's exact test a statistical test for association in a two-by-two table based on the exact hypergeometric distribution of the frequencies within the table. . Mathematical Modeling The potential for development of praziquantel resistance in the study population was first estimated by the Hardy-Weinberg equilibrium analysis (28). We then used a deterministic, simultaneous differential equation differential equation Mathematical statement that contains one or more derivatives. It states a relationship involving the rates of change of continuously changing quantities modeled by functions. model of helminth resistance (Appendix, 29). This more advanced model takes into account the skewed skewed curve of a usually unimodal distribution with one tail drawn out more than the other and the median will lie above or below the mean. skewed Epidemiology adjective Referring to an asymmetrical distribution of a population or of data (negative binomial binomial (bī'nō`mēəl), polynomial expression (see polynomial) containing two terms, for example, x+y. The binomial theorem, or binomial formula, gives the expansion of the nth power of a binomial (x+ ) distribution of number of worms in human populations, the obligate obligate /ob·li·gate/ (ob´li-gat) pertaining to or characterized by the ability to survive only in a particular environment or to assume only a particular role, as an obligate anaerobe. sexual reproduction sexual reproduction n. Reproduction by the union of male and female gametes to form a zygote. Also called syngenesis. of the parasites, and a possible decrease in fecundity fecundity /fe·cun·di·ty/ (fe-kun´dit-e) 1. in demography, the physiological ability to reproduce, as opposed to fertility. 2. ability to produce offspring rapidly and in large numbers. as a result of parasite crowding in heavily infected humans. The model provides estimates of average level of infection in the study population, as well as the prevalence and density of resistant worms over time. Results are shown as three-dimensional graphs of mean numbers of worms over time (20 years), as a function of annual community drug use (p), and the reproductive fitness of resistant parasites. Treatment efficacy and aggregation constants for infection (k) were derived from our study area. Results Yearly Efficacy of Praziquantel During 1984 to 1992, we observed substantial year-to-year variations in cure rates (conversion from egg-positive to egg-negative status on urine Nuclepore filtration examination) for both praziquantel and metrifonate (Table 1). The response to metrifonate treatment declined each year, from 79% in 1984 to 47% in 1987 (p [is less than] 0.001, Figure 1); in contrast, we observed no consistent downward trend in response to praziquantel treatment, despite repeated use of the drug in many patients (Figures 1 and 2). However, the response to praziquantel varied significantly from year to year (p [is less than] 0.001), from a cure rate of 96% in 1990 (year 7 of the project) to a cure rate of 65% in 1986 (year 3, p [is less than] 0.001). This level of efficacy was within the previous range of S. haematobium cure rates, both in Coast Province and elsewhere in Africa (Table 2). In suppression of infection intensity, the praziquantel-mediated reduction of mean S. haematobium egg counts was consistently [is greater than or equal to] 83% for all years of observation. [Figures 1-2 ILLUSTRATION OMITTED] Table 1. Effectiveness of praziquantel in eliminating Schistosoma haematobium infection, Msambweni, Coast Province, Kenya, 1984-1992
Prevalence of infection
at 12 months after
treatment
(interval change in
geometric mean of (egg
count + 1) for group)
Year treated with PZQ or
metrifonate
Patient's
infection and
treatment status 1984 1985
Egg-positive urine, 17% 12%
Given PZQ, never (97 to 1.5) (33 to 1.5)
previously treated n = 981 n = 51
Egg-positive urine, -- 13%
Given PZQ, had [is greater (10 to 1.5)
than or equal to 1] n = 111
PZQ treatments
All egg-positive, 17% 13%
PZQ-treated patients (97 to 1.5) (15 to 1.5)
n = 981 n = 162
Infection rate 15% 9%
(egg - to egg + conversion)
All patients, treated and 18% 12%
untreated n = 3,196 n = 2,498
Prevalence of infection at 12 months
after treatment
(interval change in geometric mean
of (egg count + 1) for group)
Year treated with PZQ or metrifonate
Patient's
infection and
treatment status 1986 1987 1989
Egg-positive urine, 34% -- 15%
Given PZQ, never (29 to 3.7) (18 to 1.5)
previously treated n = 82 n = 352
Egg-positive urine, 38% -- 10%
Given PZQ, had [is greater (16 to 2.6) (19 to 1.1)
than or equal to 1] n = 47 n = 68
PZQ treatments
All egg-positive, 35% -- 14%
PZQ-treated patients (24 to 3.3) (19 to 1.4)
n = 129 n = 420
Infection rate 11% 11% 13%
(egg - to egg + conversion)
All patients, treated and 14% 19% 14%
untreated n = 2,372 n = 1,968 n = 1,398
Prevalence of infection
at 12 months after
treatment
(interval change in
geometric mean of (egg
count + 1) for group)
Year treated with PZQ or
metrifonate
Patient's
infection and
treatment status 1990 1991
Egg-positive urine, 4% 35%
Given PZQ, never (22 to 1.1) (24 to 4)
previously treated n = 292 n = 274
Egg-positive urine, 29% 2%
Given PZQ, had [is greater (13 to 2.8) (14 to 1.0)
than or equal to 1] n = 64 n = 73
PZQ treatments
All egg-positive, 4% 34%
PZQ-treated patients (20 to 1.1) (22 to 3.8)
n = 365 n = 338
Infection rate 10% 21%
(egg - to egg + conversion)
All patients, treated and 13% 24%
untreated n = 2,579 n = 1,938
PZQ = praziquantel. Table 2. Reported praziquantel (40 mg/kg) efficacy for Schistosoma haematobium, Coast Province, Kenya, and elsewhere in Africa
Cure rate(s)
Site observed (%) Year(s)
Coast Province, Kenya
Kajiwe, Kilifi district 62-65 1994
Msambweni area, Kwale district 65-96 1984-91
Southern Kwale district 84 1986
Kwale district 87 1986
Elsewhere
Senegal 80-93 1995
Ghana 67 1994
Zimbabwe 72 1986
Mauritania 90-95 1985-86
Ghana 60 1984
Egypt 59-62 1983
Gambia 57-93 1983
Tanzania 66-83 1979
Site Reference
Coast Province, Kenya
Kajiwe, Kilifi district Olds et al., 45
Msambweni area, Kwale district present study
Southern Kwale district King et al., 46
Kwale district Stephenson et al., 47
Elsewhere
Senegal Shaw et al., 48
Ghana Chan et al., 9
Zimbabwe Taylor et al, 49
Mauritania Etard et al., 50
Ghana Mott et al., 42
Egypt el Malatawy et al., 51
Gambia Wilkins et al., 52
Tanzania McMahon and Kolstrup, 53
Impact of Repeated Treatment In both the study periods during which repeated, annual praziquantel treatment was used (1984-1987 and 1989-1993), the observed cure rate for egg-positive children increased in year 2 of treatment, then decreased in year 3 (Figure 1). The number of egg-positive children remaining to be treated in successive years was small, and this sample did not have sufficient statistical power to determine whether the year 3 decrease in praziquantel response was due to fluctuations in transmission (30), progressive selection of patients at high risk for exposure to S. haematobium (27,31), or gradual selection of praziquantel-resistant parasites. Given the incomplete efficacy of praziquantel in eradicating infection (6) and the single annual follow-up, our study design could not distinguish reinfection reinfection /re·in·fec·tion/ (-in-fek´shun) a second infection by the same agent or a second infection of an organ with a different agent. re·in·fec·tion n. from possible drug failure. Therefore, we used several indirect variables to estimate ongoing praziquantel efficacy: the level of persistent egg-positivity at I year after praziquantel treatment, compared with rates of new infection (egg-negative to egg-positive conversion) each year; the efficacy of the drug in children receiving a second, third, or fourth dose, compared with efficacy in children receiving a first dose; and the efficacy of the drug in children who remained egg-positive after their first dose compared with efficacy in children whose infections cleared but who subsequently became reinfected. Persistent Infection vs. Reinfection The yearly efficacy of praziquantel treatment and infection or reinfection rates (egg-negative to egg-positive conversion) were compiled for the study population (Table 1). Yearly infection or reinfection rates varied from 15% in 1984 to 1985 to a low of 9% in 1985 to 1986 and a high of 21% in 1991 to 1992 (average 13%). Infection rates for children initially treated with praziquantel who subsequently missed I year or more of treatment were 22% to 34% in subsequent surveys 2 to 4 years later. These rates suggested a time-dependent average accumulation of reinfection at an annual rate of 9% to 15%. The high transmission levels in 1991 to 1992 (21% new infection or reinfection) may explain the apparent decrease in praziquantel efficacy during this 12-month period. However, estimated transmission did not explain the decreased efficacy seen in 1986 to 1987, when the population egg-negative to -positive conversion rate was only 11%. Efficacy of Retreatment with Praziquantel To examine whether an increasing core of resistant infection might account for the higher post-treatment prevalence after year 2 of treatment, we compared the relative annual efficacy in egg-positive patients who received praziquantel for the first time with efficacy in patients receiving their second, third, or fourth treatments. We found that after the first cycle of treatment, i.e., from 1985 on, praziquantel-mediated cure rates did not differ for patients with first-time treatment and those with a history of praziquantel treatment (Figure 2). We further examined the response to second, third, and fourth treatments in patients who did not become egg-negative after their first dose (i.e., initial nonresponse, possibly resistant) (Figure 3). We compared these results with those of patients who tested negative after the first praziquantel dose, then became egg-positive in later years (those reinfected after cure, Figure 3). Children from these two groups, who were at greatest risk for infection with resistant parasites, eventually reverted to egg-negative status after treatment with one to three supplemental praziquantel doses. The two groups did not differ significantly in their response rates to the second, third, or fourth doses. [Figure 3 ILLUSTRATION OMITTED] Discussion Without clear evidence of emerging resistance in our treated population, we considered two related questions: Why was resistance not observed, and when might it be expected to emerge under the field conditions tested? To answer these questions, we turned to mathematical models of inheritance of drug resistance. A number of factors may account for the lack of evidence of praziquantel resistance in the Msambweni project. Although S. haematobium resistance to praziquantel is likely to emerge at some future time, the interval required for detection of resistance may be much longer than our 8-year observation period. An effective praziquantel-resistance mutation may be so rare that the number of generations required for it to become the dominant phenotype has not yet occurred. In Egypt, for example, apparently resistant strains of S. mansoni are emerging [is greater than] 10 years after widespread availability of praziquantel treatment (32). For a single resistance gene mutation Noun 1. gene mutation - (genetics) a mutation due to an intramolecular reorganization of a gene point mutation genetic science, genetics - the branch of biology that studies heredity and variation in organisms beginning at frequency of [10.sup.-6], a Hardy-Weinberg equilibrium analysis (28) predicts it would take eight or more generations for the resistant phenotype to become clinically detectable (i.e., 25% to 50% of worms) at the community treatment rates used in this study, if the resistance gene heterozygotes are fully resistant to treatment (i.e., a dominant trait dominant trait n. An inherited character determined by a dominant gene. Also called dominant character. Dominant trait [Figure 4a1). In our study, we estimate that 25% to 50% of infections were treated, but because the targeted school-age groups have the highest numbers of worms, 50% to 75% of worms may have been exposed to praziquantel. Emergence times for the resistance phenotype are longer if heterozygotes remain fully or partially susceptible to the drug (11 generations for 25% heterozygote heterozygote (hĕt'ərōzī`gōt): see genetics. loss after treatment and 14 to 18 generations for 50% heterozygote losses) and only the homozygotes are fully resistant (Figure 4b). Given the seasonal nature of rainfall and water exposure, the requirement of two sexes for schistosome reproduction, and the uneven aggregation of worms in the human population, the effective generation time for S. haematobium is likely to be at least 6 to 12 months, so we observed no more than 8 to 16 generations; our observation period may have been too short to identify praziquantel resistance. Our annual follow-up was an insensitive means to detect drug failure due to resistance. However, under the pressure of continued praziquantel treatment in the community, if resistant worms are fully fit, rapid predominance of resistant strains would be expected (Figure 4). [Figure 4 ILLUSTRATION OMITTED] Praziquantel failure on initial treatment in S. mansoni-endemic areas of Senegal suggests primary resistance to praziquantel (16,18) and a high prevalence of resistance genes in the local S. mansoni strain (21,33,34). More recent reports indicate, however, that in this area of Senegal, retreatment after 40 days adequately reduces infection levels and achieves better cure rates (19). The latter results suggest that immature schistosomes, which are known not to be susceptible to praziquantel, are typically present in Senegalese patients at the time of treatment. If the treated patient has been recently exposed to infection ([is less than or equal to] 6 weeks ago) in an area with continuous--rather than seasonal--transmission, apparent treatment failure may be observed when unaffected juvenile worms reach maturity and pass eggs several weeks after praziquantel treatment (14). Annual reinfection rates for S. haematobium may be high in some areas, such as Niger (35), and post-treatment infection detected after a single round of therapy should not be immediately interpreted as evidence of praziquantel resistance. Nevertheless, animal studies of S. mansoni strains from Senegal indicate they are less sensitive to praziquantel than strains from other parts of the world (21,33,34). There is another explanation for an apparent low-level prevalence of drug resistance that fails to predominate in the parasite population: if a praziquantel-resistance mutation compromises reproductive fitness, the homozygous ho·mo·zy·gous adj. Having the same alleles at one or more gene loci on homologous chromosome segments. Homozygous Identical genes controlling a specified inherited trait. , fully resistant worm will never predominate. Instead, under the pressure of continued treatment, the resistance gene will achieve a stable-equilibrium share of the worm population, at a level dependent on its lower survival efficiency relative to that of the praziquantel-sensitive genotype (Figure 4c). This situation is analogous to the effect of the sickle cell-hemoglobin gene in human populations exposed to malaria. Another possible factor likely to be slowing the emergence of praziquantel resistance in Schistosoma is the parasite's obligate diecious sexual reproduction. Unlike drug-resistant bacteria, praziquantel-resistant schistosomes must find a mate of the opposite sex to reproduce, which requires a sufficient density of human infection. In a disease-endemic area where most of the population has been treated, the initial heavy loss of susceptible worms (>80%) may actually reduce mean number of worms sufficiently (i.e., to fewer than one male and one female per host) to prevent most resistant worms from finding suitable mates (29). Worm distribution is highly aggregated in the human population, with most (75%) patients having light infections and a small proportion (approximately 5%) having heavy infections. Heavy infection can result in reduced worm fecundity, slowing the production of eggs and thus the transmission of genes from a resistant worm, even though the chances of mating are enhanced. After treatment, the reduced number of worms in a heavily infected human could increase fecundity, so the net effect of treatment on praziquantel-resistance gene transmission would be difficult to predict. In an age-targeted program such as ours, praziquantel-sensitive parasites would also persist in Verb 1. persist in - do something repeatedly and showing no intention to stop; "We continued our research into the cause of the illness"; "The landlord persists in asking us to move" continue the untreated adult and infant human subpopulations, slowing the dominance of drug resistance gene(s). This would occur by allowing interbreeding interbreeding crossbreeding, as between half-breds. of resistant and susceptible worms in host locations not having the environmental pressure (i.e., praziquantel treatment) that favors the resistance gene. Using a dynamic model of parasite transmission that accounts for these reproductive features of macroparasite transmission (Appendix), we examined the impact of treatment coverage and duration of control programs on the emergence of resistant infection, to estimate the time required for drug failure. We also examined the impact of varying reproductive fitness of the resistant worms on the time to recrudescence recrudescence /re·cru·des·cence/ (re?kroo-des´ens) recurrence of symptoms after temporary abatement.recrudes´cent re·cru·des·cence n. of infection. Figures 5 and 6 show the predicted recrudescence of infection over a 20-year period, as influenced by treatment coverage and by reproductive fitness of resistant worms. Both simulations indicate at least an 8- to 10-year delay in the return of infection to pretreatment pretreatment, n the protocols required before beginning therapy, usually of a diagnostic nature; before treatment. pretreatment estimate, n See predetermination. levels. This delay is especially noted if treatment coverage is incomplete (Figure 5) and resistant parasites are less reproductively fit than susceptible ones (Figure 6). The model further indicates that under the conditions of our program (targeted mass treatment, with 25% to 75% of infections praziquantel-treated), resistance becomes clinically apparent ([is greater than] 50% resistant worms) only after a period years longer than that we were able to observe. [Figures 5-6 ILLUSTRATION OMITTED] In our model, we assumed an effective spontaneous mutation spontaneous mutation n. A mutation that arises naturally and not as a result of exposure to mutagens. Also called natural mutation. rate for praziquantel resistance of [10.sup.-6]. Recent work by Moxon and colleagues (36-38) on the evolution of bacterial pathogens indicates that genetic mutation Noun 1. genetic mutation - (genetics) any event that changes genetic structure; any alteration in the inherited nucleic acid sequence of the genotype of an organism chromosomal mutation, mutation becomes accelerated (i.e., nonrandom) in a subset of organisms under environmental stress, such as drug pressure. The "hypermutable" phenotype prevails under these rapidly changing conditions because of its ability to adapt quickly to the new environment. Rapid genetic diversification is enhanced by simultaneous modular changes in DNA DNA: see nucleic acid. DNA or deoxyribonucleic acid One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes. , which are facilitated by the presence of multiple copies of critical genes, transposons Transposons Types of transposable elements which comprise large discrete segments of deoxyribonucleic acid (DNA) capable of moving from one chromosome site to a new location. , and repeat regions or Z-DNA boundaries flanking key intron/exon boundaries (39). Higher organisms, such as schistosomes, are likely to use similar mechanisms in adaptation. Drake (40) has estimated that the effective spontaneous mutation rate per genome per sexual generation may be as high as [10.sup.-2] for the nematode nematode or roundworm Any of more than 15,000 named and many more unnamed species of worms in the class Nematoda (phylum Aschelminthes). Nematodes include plant and animal parasites and free-living forms found in soil, freshwater, saltwater, and even vinegar C. elegans C. elegans A nematode (Caenorhabditis elegans) that lives in soil, feeds on bacteria, and reaches lengths of about 1 mm (0.04 inch). It was the first animal whose genome was completely sequenced, and is widely used as a "model organism" by and [10.sup.-1] for the insect Drosophila Drosophila: see fruit fly. drosophila Any member of about 1,000 species in the dipteran genus Drosophila, commonly known as fruit flies but also called vinegar flies. Some species, particularly D. . In sensitivity analysis of our differential model, reducing the mutation rate In genetics, the mutation rate is the chance of a mutation occurring in an organism or gene in each generation (or, in the case of multicellular organisms, cell division). See Luria-Delbrück experiment. from [10.sup.-6] to [10.sup.-1] in our base case (50% coverage with 85% efficacy) reduced the expected time to emergence of resistance from 10 to 7 years. At higher levels of drug use (90%-100% coverage), the time to resistance was reduced from 7 to 5 years at the highest mutation rate ([10.sup.-1]). This effect is not as dramatic as would be predicted by the simpler Hardy-Weinberg model (i.e., a reduction from 14 to 3 generations for dominance of resistance), apparently because of the retarding effects of aggregation and mating on emergence of new genotypes. In summary, our results indicate that significant resistance to praziquantel treatment had not emerged in S. haematobium in the Msambweni area as of 1991. As noted since its first use, praziquantel treatment was not 100% effective in eliminating infection (41). It was, however, reliably capable of suppressing intensity of infection in each of six rounds of treatment spaced over 8 years. These findings, together with our modeling analysis, support targeted use of chemotherapy for disease control in S. haematobium-endemic populations (1,26,4244). In our program, praziquantel treatment was focused only on schoolchildren, the subpopulation sub·pop·u·la·tion n. A part or subdivision of a population, especially one originating from some other population: microbial subpopulations. Noun 1. having the highest numbers of worms (26,27). Higher treatment coverage increases evolutionary pressure Evolutionary pressure or selection pressure can be formalized as an external pressure applied to a process, thereby pushing that process in a distinct direction. on the schistosome population and hastens emergence of resistance. The limited coverage of a targeted (vs. mass-treatment) program may have reduced the tendency for resistance to emerge, compared with the experience reported for S. mansoni in Egypt (32). For the treated Msambweni population, the benefits of treatment appeared to be maximal after 2 years of repeated yearly treatment (26,27). After this, a 2- to 3-year interval may be sufficient to maintain effective suppression of infection and disease (27). Because reduced exposure to the drug slows the emergence of drug resistance, the efficacy of longer intertreatment intervals in suppressing S. haematobium-related disease should be studied. Although efficacy should be maintained for a number of years, regular monitoring of drug efficacy is appropriate for all long-term praziquantel-based control programs (14). Emergence of praziquantel resistance should be anticipated within 10 to 20 years, and continued antischistosomal drug development should be pursued. Acknowledgments We thank the staff of the Division of Vector Borne Diseases, Ministry of Health, Kenya, and the students, residents, and faculty of Case Western Reserve University who worked to make the Msambweni Study a success; the people of the Msambweni area of Kwale District for their enthusiastic participation; and Daren Austin for his description and helpful discussions of macroparasite resistance models. This work was supported by grants from the Edna McConnell Clark Foundation, the WHO-TDR/UNDP Research Training Program, and the National Institutes of Health (AI 33061, AI45473). Dr. King is an associate professor of Medicine and International Health at Case Western Reserve University in Cleveland, Ohio "Cleveland" redirects here. For the Cleveland metropolitan area, see . For other uses, see Cleveland (disambiguation). Cleveland is a city in the U.S. state of Ohio and the county seat of Cuyahoga County, the most populous county in the state. . His current research focuses on modeling of transmission of infectious diseases infectious diseases: see communicable diseases. and prevention of disease due to helminthic hel·min·thic adj. 1. Of or relating to worms, especially parasitic worms. 2. Tending to expel worms. n. See anthelmintic. infection. References (1.)World Health Organization. The control of schistosomiasis: second report of the WHO Expert Committee. Vol. 830 Geneva Geneva, canton and city, Switzerland Geneva (jənē`və), Fr. Genève, canton (1990 pop. 373,019), 109 sq mi (282 sq km), SW Switzerland, surrounding the southwest tip of the Lake of Geneva. : 1993 WHO Technical Report. (2.)Drugs for parasitic infections. Med Lett Drugs Ther 1998;40:1-12. (3.)Hotez PJ, Zheng F, Long-qi X, Ming-gang C, Shu-hua X, Shu-xian L, et al. Emerging and reemerging helminthiases and the public health of China. Emerg Infect Dis 1997;3:303-10. (4.)Praziquantel. USP USP - unique sales point Drug Information. Vol. I. Rockville, MD: United States United States, officially United States of America, republic (2005 est. pop. 295,734,000), 3,539,227 sq mi (9,166,598 sq km), North America. The United States is the world's third largest country in population and the fourth largest country in area. Pharmacopeial phar·ma·co·pe·ial adj. 1. Of or relating to a pharmacopoeia. 2. Relating to a drug in the list of the United States Pharmacopoeia or similar pharmacopoeia. Convention; 1998:2395-7. (5.) King CH, Mahmoud AA. Drugs five years later: praziquantel. Ann Intern Med 1989;110:290-6. (6.) Davis A, Wegner DH. Multicentre trials of praziquantel in human schistosomiasis: design and techniques. Bull WHO 1979;57:767-71. (7.) Brindley PJ. Drug resistance to schistosomicides and other anthelmintics of medical significance. Acta Trop 1994;56:213-31. (8.) Boisier P, Ramarokoto CE, Ravaoalimalala VE, Rabarijaona L, Serieye J, Roux Roux , Pierre Paul Émile 1853-1933. French bacteriologist. His work with the diphtheria bacillus led to the development of antitoxins to neutralize pathogenic toxins. J, et al. Reversibility of Schistosoma mansoni-associated morbidity after yearly mass praziquantel therapy: ultrasonographic assessment. Trans R Soc Trop Med Hyg 1998;92:451-3. (9.) Chan MS, Nsowah-Nuamah NNN NNN Triple Net (method of computing real estate costs among commercial rental properties; lease) NNN Nippon News Network (Japan) NNN Newspaper National Network LP NNN Novy-MacNeal-Nicolle , Adjei S, Wen S, Hall A, Bundy DAP. Predicting impact of school-based treatment for urinary schistosomiasis given by the Ghana Partnership for Child Development. Trans Roy Soc Trop Med Hyg 1998;92:386-9. (10.) Jongsuksuntigul P, Imsomboon T. The impact of a decade long opisthorchiasis control program in northeastern Thailand. Southeast Asian J Trop Med Public Health 1997;28:551-7. (11.) Schelling U, Frank W, Will R, Romig T, Lucius R. Chemotherapy with praziquantel has the potential to reduce the prevalence of Echinococcus multilocularis Echinococcus multilocularis is a cyclophyllid cestode that, like Echinococcus granulosus, produces hydatid disease in many mammals, including rodents and humans. Unlike E. in wild foxes (Vulpes vulpes Vulpes vulpes see red fox. ). Ann Trop Med Parasitol 1997;91:179-86. (12.) Llayd S, Walters TM. Worming of dogs in mid-Wales for Echinococcus granulosus Echinococcus granulosus, also called the Hydatid worm, is a cyclophyllid cestode that parasitizes the small intestine of canids as an adult, but which has important intermediate hosts such as livestock and humans, where it causes hydatid disease. . Vet Rec 1997; 140:487-8. (13.) Olveda RM, Daniel BL, Ramirez BD, Aligui GD, Acosta LP, Fevidal P, et al. Schistosomiasis japonica japonica (jəpŏn`əkə): see quince; camellia. in the Philippines: the long-term impact of population-based chemotherapy on infection, transmission, and morbidity. J Infect Dis 1996;174:163-72. (14.) Renganathan E, Cioli D. An international initiative on praziquantel use. Parasitol Today 1998;14:390-1. (15.) Kusel J, Hagan P. Praziquantel--its use, cost and possible development of resistance [news]. Parasitol Today 1999; 15:352-4. (16.) Guisse F, Polman K, Stelma FF, Mbaye A, Talla I, Niang M, et al. Therapeutic evaluation of two different dose regimens of praziquantel in a recent Schistosoma mansoni Schistosoma man·so·ni n. A trematode that is common in Africa, parts of the Middle East, the West Indies, South America, and certain Caribbean islands and causes schistosomiasis mansoni. focus in Northern Senegal. Am J Trop Med Hyg 1997;56:511-4. (17.) Stelma FF, Sall S, Daff B, Sow S, Niang M, Gryseels B. Oxamniquine cures Schistosoma mansoni infection in a focus in which cure rates with praziquantel are unusually low. J Infect Dis 1997;176:304-7. (18.) Stelma FF, Talla I, Sow S, Kongs A, Niang M, Polman K, et al. Efficacy and side effects of praziquantel in an epidemic focus of Schistosoma mansoni. Am J Trop Med Hyg 1995;53:167-70. (19.) Picquet picquet: see piquet. M, Vercruysse J, Shaw DJ, Diop M, Ly A. Efficacy of praziquantel against Schistosoma mansoni in northern Senegal. Trans R Soc Trop Med Hyg 1998;92:90-3. (20.) Bennett JL, Day T, Feng-Tao L, Ismail M, Farghaly A. The development of resistance to anthelmintics: A perspective with an emphasis on the antischistosomal drug praziquantel. Exp Parasitol 1997;87:260-7. (21.) Fallon PG, Mubarak JS, Fookes RE, Niang M, Butterworth AE, Sturrock RF, et al. Schistosoma mansoni: maturation rate and drug susceptibility of different geographic isolates. Exp Parasitol 1997;86:29-36. (22.) Pereira C, Fallon PG, Cornette J, Capron A, Doenhoff MJ, Pierce RJ. Alterations in cytochrome-c oxidase oxidase /ox·i·dase/ (ok´si-das) any enzyme of the class of oxidoreductases in which molecular oxygen is the hydrogen acceptor. ox·i·dase n. expression between praziquantel-resistant and susceptible strains of Schistosoma mansoni. Parasitology Parasitology The scientific study of parasites and of parasitism. Parasitism is a subdivision of symbiosis and is defined as an intimate association between an organism (parasite) and another, larger species of organism (host) upon which the parasite is 1998;117:63-73. (23.) Cunha VM, Noel F. (Ca(2+)-Mg2+)ATPase in Schistosoma mansoni: evidence for heterogeneity and resistance to praziquantel. Mem Inst Oswaldo Cruz Oswaldo Gonçalves Cruz, better know as Oswaldo Cruz (pron. IPA: [osvawdu cɾuz]), (b. August 5, 1872, São Luíz de Paraitinga, São Paulo state, Brazil; d. 1998;93:181-2. (24.) Cioli D, Pica Mattoccia L. Genetic analysis of hycanthone resistance in Schistosoma mansoni. Am J Trop Med Hyg 1984;33:80-8. (25.) King CH, Lombardi G, Lombardi C, Greenblatt R, Hodder S, Kinyanjui H, et al. Chemotherapy-based control of schistosomiasis haematobia. I. Metrifonate versus praziquantel in control of intensity and prevalence of infection. Am J Trop Med Hyg 1988;39:295-305. (26.) King CH, Muchiri EM, Ouma ouma Noun S African 1. grandmother, often as a title with a surname 2. Slang any elderly woman [Afrikaans] JH. Age-targeted chemotherapy for control of urinary schistosomiasis in endemic populations. Mem Inst Oswaldo Cruz 1992;87:203-10. (27.) Muchiri EM, Ouma JH, King CH. Dynamics and control of Schistosoma haematobium transmission in Kenya: an overview of the Msambweni Project. Am J Trop Med Hyg 1996;55:127-34. (28.) Khoury MJ, Beaty TH, Cohen cohen or kohen (Hebrew: “priest”) Jewish priest descended from Zadok (a descendant of Aaron), priest at the First Temple of Jerusalem. The biblical priesthood was hereditary and male. BH. Fundamentals of genetic epidemiology. New York New York, state, United States New York, Middle Atlantic state of the United States. It is bordered by Vermont, Massachusetts, Connecticut, and the Atlantic Ocean (E), New Jersey and Pennsylvania (S), Lakes Erie and Ontario and the Canadian province of : Oxford University Press; 1993. (29.) Anderson RM, May RM. Infectious diseases of humans: dynamics and control. New York: Oxford University Press; 1991:467-96, 507-20. (30.) Sturrock RF, Kinyanjui H, Thiongo FW, Tosha S, Ouma JH, King CH, et al. Chemotherapy-based control of schistosomiasis haematobia. 3. Snail studies monitoring the effect of chemotherapy on transmission in the Msambweni area, Kenya. Trans R Soc Trop Med Hyg 1990;84:257-61. (31.) Muchiri EM. Association of water contact activities and risk of reinfection for S. haematobium after drug treatment in the Msambweni Area, Kenya [MS thesis, Epidemiology and Biostatistics]. Case Western Reserve University; 1991. (32.) 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Appendix The following system of differential equations was used to model the level of schistosome infection and prevalence of resistant worms in the treated study population, where [Sigma] is the number of sensitive schistosomes per host, [Rho] is the number of resistant schistosomes per host, and [Sigma] + [Rho] = M, the mean number of worms per host. If p = the proportion of treated infections each year, and h = the efficacy of one course of treatment, then c = - ln (1- ph) is the relative increase in the per capita [Latin, By the heads or polls.] A term used in the Descent and Distribution of the estate of one who dies without a will. It means to share and share alike according to the number of individuals. death rate of sensitive worms due to treatment. The basic death rate for sensitive and resistant parasites is an aggregate function of parasite and host death rates, represented in the equations as [[Gamma].sub.s] = 1/sensitive parasite lifespan + 1/host lifespan and [[Gamma].sub.r] = 1/resistant parasite lifespan + 1/host lifespan [R.sub.0] represents the basic reproductive rate of the susceptible worm. If [Phi] = the relative loss of reproductive fitness of the resistant phenotype (with value from 0 to 1), then [R.sub.0r] = [R.sub.0] (1 - [Phi]). X represents the spontaneous mutation rate of resistant worms. To reflect the impact of obligate sexual mating and unequal distribution of worms among hosts, F is a fecundity expression where [Psi] = the mating probability, z = the density-dependent effect on worm fecundity, and k = the aggregation constant of the negative binomial distribution In probability and statistics the negative binomial distribution is a discrete probability distribution. The Pascal distribution and the Polya distribution are special cases of the negative binomial. of worms, such that F ([Sigma] + [Rho]) = [Psi] [[1 + ([Sigma] + [Rho]) (1 - z)/k].sup.-(k + 1)] Then, along the lines of equation 17.5 of Anderson and May (29) for repeated treatment, [MATHEMATICAL EXPRESSION A group of characters or symbols representing a quantity or an operation. See arithmetic expression. NOT REPRODUCIBLE IN ASCII ASCII or American Standard Code for Information Interchange, a set of codes used to represent letters, numbers, a few symbols, and control characters. Originally designed for teletype operations, it has found wide application in computers. ] and assuming resistant parasites to be completely unaffected by treatment, [MATHEMATICAL EXPRESSION NOT REPRODUCIBLE IN ASCII] For the numerical analysis of these equations, we used the ODE solver of MathCAD (MathSoft, Inc., Cambridge MA) based on the Runge-Kutta estimation with 1,000 steps for a model time span of 20 years. Initial variable estimates were taken from our field data (treatment coverage among total infected population, p = 0.25 to 0.75; treatment efficacy, h = .65 to .95; aggregation constant, k = 0.067; host lifespan = 50 years) or from previously published estimates for S. haematobium biology ([R.sub.0] = 2 to 4; parasite lifespan = 3 to 5 years; density effect on fecundity, z = 0.96 to 0.99) (29). Address for correspondence: Charles H. King, Division of Geographic Medicine, Room W137, Case Western Reserve University School of Medicine, 10900 Euclid Avenue, cleveland, Ohio, USA 44106-4983; Fax: 216-368-4828; e-mail: chk@po.cwru.edu. Charles H. King,[*] Eric M. Muchiri,([dagger]) and John H. Ouma([dagger]) [*] Case Western Reserve University School of Medicine and University Hospitals of Cleveland, Cleveland, Ohio, USA; and ([dagger]) Ministry of Health, Nairobi, Kenya |
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