Treatment and education reduce the severity of
					schistosomiasis periportal fibrosis

Silva, Paula Carolina Valença; Leal, Tallita Veríssimo; Domingues, Ana Lúcia Coutinho

doi:10.1590/0037-8682-0110-2013

Abstract

Introduction

This study evaluates the factors associated with the development of severe periportal fibrosis in patients with Schistosoma mansoni.

Methods

A cross-sectional study was conducted from April to December 2012 involving 178 patients infected with S. mansoni who were treated in the Hospital das Clínicas of Pernambuco, Brazil. Information regarding risk factors was obtained using a questionnaire. Based on the patients' epidemiological history, clinical examination, and upper abdomen ultrasound evaluation, patients were divided into 2 groups: 137 with evidence of severe periportal fibrosis and 41 patients without fibrosis or with mild or moderate periportal fibrosis. Univariate and multivariate analyses were conducted using EpiInfo software version 3.5.5.

Results

Illiterate individuals (30.1%) and patients who had more frequent contact with contaminated water in towns in the Zona da Mata of Pernambuco (33.2%) were at greater risk for severe periportal fibrosis. Based on multivariate analysis, it was determined that an education level of up to 11 years of study and specific prior treatment for schistosomiasis were preventive factors for severe periportal fibrosis.

Conclusions

The prevailing sites of the severe forms of periportal fibrosis are still within the Zona da Mata of Pernambuco, although there has been an expansion to urban areas and the state coast. Specific treatment and an increased level of education were identified as protective factors, indicating the need for implementing social, sanitary, and health education interventions aimed at schistosomiasis to combat the risk factors for this major public health problem.

Schistosomiasis mansoni; Periportal fibrosis; Epidemiology

INTRODUCTION

Schistosoma mansoni is a major public health problem worldwide that has great social and economic impact. The disease affects over 200 million people around the world. Approximately 6 million people are infected in Brazil, particularly in the Northeast region¹1. World Health Organization (WHO). Programs and projects: schistosomiaisis. A major public health. 2010. [Cited 2010 February 25]. Available at: http://www.who.int/schistosomiaisis/en/.
http://www.who.int/schistosomiaisis/en/... –³3. Katz N, Peixoto SV. Análise crítica da estimativa do número de portadores de esquistossomose mansoni no Brasil. Rev Soc Bras Med Trop 2000; 33:303-308..

One characteristic of this disease is the capacity to cause an inflammatory response against the Schistosoma mansoni eggs deposited in the host's liver. This process can lead to periportal fibrosis (PPF) due to the deposition and accumulation of extracellular matrix, causing the host to develop portal hypertension that leads to splenomegaly and the emergence of varicose veins in the esophagus. Rupture of these esophageal varices with subsequent severe gastrointestinal bleeding occurs in 12 to 15% of patients, which leads to death in approximately 20% of cases⁴4. Prata A, Ruiz-Guevara R, Antunes CMF, Marinho CC, Queiroz LC, Voieta I, et al. Comparação entre achados clínicos e ultrassonográficos no diagnóstico da fibrose periportal em uma área endêmica de esquistossomose no Brasil. Rev Soc Bras Med Trop 2010; 43:129-134.–⁶6. Andrade ZA. Schistosomiasis and liver fibrosis. Parasite Immunology 2009, 31:656-663..

The disease presents in various clinical forms, with 5% to 10% of individuals developing severe liver and spleen lesions the hepatosplenic form described above of which schistosomal fibrosis is among the most important aspects⁷7. Henri S, Chevillard C, Mergani A, Paris P, Gaudart J, Camilla C, et al. Cytokine regulation of periportal fibrosis in humans infected with Schistosoma mansoni: IFN-gamma is associated with protection against fibrosis and TNF-alpha with aggravation of disease. J Immunol 2002; 169:929-936.. The risk for developing the most severe hepatosplenic form of schistosomiasis increases according to the severity of the fibrosis⁶6. Andrade ZA. Schistosomiasis and liver fibrosis. Parasite Immunology 2009, 31:656-663.,⁸8. Domingues AL, Lima AR, Dias HS, Leão GC, Coutinho A. Na ultrasonographic study of liver fibrosis in patients infected with Schistosoma mansoni in northeast Brazil. Trans R Soc Trop Med Hyg 1993; 87:555-558..

One factor related to PPF is the infection intensity. Several factors are related to the occurrence of schistosomal infection, including exposure time, frequency of contact with contaminated water, and age at infection. Different contacts with contaminated water bodies (natural waters, stream waters, water reservoirs) may determine different epidemiological patterns of infection and transmission⁹9. Araujo KCGM, Resendes APC, Souza-Santos R, Silveira Júnior JC, Barbosa CS. Análise espacial dos focos de Biomphalaria glabrata e de casos humanos de esquistossomose mansônica em Porto de Galinhas, Pernambuco, Brasil, no ano 2000. Cad Saude Publica 2007; 23:409-417.. Thus, understanding the evolution of the various clinical forms of schistosomiasis involves understanding a set of factors, such as poor housing and sanitation conditions, economic and sociocultural activities related to the use of contaminated water in rural areas, lack of health education, low adherence to control programs, and lack of an effective vaccine, all of which have contributed to morbidity¹⁰10. Pordeus LC, Aguiar LR, Quinino LRM, Barbosa CS. A ocorrência das formas aguda e crônica da esquistossomose mansônica no Brasil no período de 1997 a 2006: uma revisão de literatura. Epidemiol Serv Saude 2008,17:163-175.. Other factors, such as the exacerbation of the host's immune response, concomitant infections, virulence of the S. mansoni strain, and nutritional status of infected individuals, should be taken into account when determining an individual's susceptibility to developing the severe clinical form of the disease⁵5. Abath FGC, Morais CNL, Montenegro CEL, Wynn TA, Montenegro SML. Immunopathogenic mechanisms in schistosomiasis: what can be learnt from human studies? Trends Parasitol 2006; 22:85-91.,¹¹11. Dessein A, Chevillard C, Arnaud V, Hou X, Hamdoun AA, Dessein H, et al. Variants of CTGF are associated with hepatic fibrosis in chinese, sudanese, and brazilians infected with schistosomes. J Exp Med 2009; 12:1-8..

Currently, the mechanism of liver fibrosis has been an object of extensive research, but much work still remains to better understand the complex mechanisms related to the inhibitory and activating pathways involved in schistosomal fibrosis. Thus, understanding the causal factors that can affect the clinical outcome of this disease remains a challenge¹¹11. Dessein A, Chevillard C, Arnaud V, Hou X, Hamdoun AA, Dessein H, et al. Variants of CTGF are associated with hepatic fibrosis in chinese, sudanese, and brazilians infected with schistosomes. J Exp Med 2009; 12:1-8.–¹³13. Joshi VA, Roberts AE, Kucherlapati R. Towards a Treatment for RAS-MAPK pathway disorders. In: Zenker M, editor. Syndrome and related disorders: A matter of deregulated ras signaling. Monographs in human genetics: Basel Karger; 2008. p. 151-164.. Therefore, this study aims to describe the epidemiological and clinical factors and to evaluate the factors associated with the development of moderate to severe PPF.

METHODS

A cross-sectional study examining associations between several factors and the development of moderate to severe PPF was conducted from April to December 2012 and involved 178 patients infected with S. mansoni aged over 18 years and treated in the Gastroenterology Outpatient Clinic of Hospital das Clínicas/Universidade Federal de Pernambuco (HC/UFPE), a reference center for the treatment of schistosomiasis.

Selection of patients

All patients infected with S. mansoni examined during the study period were included. We excluded individuals with other previous liver-associated diseases, such as liver cirrhosis, steatosis, hepatitis B or C, and other clinical forms of diagnosed schistosomiasis. In total, 178 individuals were selected for the study and were divided into two groups. Group 1: 137 cases of individuals with the hepatosplenic (HS) form of the disease and Group 2: controls 41 cases of individuals with the hepatointestinal (HI) form of the disease (Figure 1).

FIGURE 1
Diagram depicting patient enrollment and classification.

The two groups were prospectively selected during the study period according to the following criteria: patients with HI schistosomiasis without splenomegaly and with mild or moderate periportal fibrosis (pattern C or D from Niamey's classification¹⁴14. Richter J, Domingues AL, Barata CH, Prata AR, Lambertucci JR. Report of the second satellite symposium on ultrasound in schistosomiasis. Mem Inst Oswaldo Cruz 2001; 96:151-156.) or those with no fibrosis and patients with HS schistosomiasis with advanced periportal fibrosis (pattern E or F from Niamey's classification¹⁴14. Richter J, Domingues AL, Barata CH, Prata AR, Lambertucci JR. Report of the second satellite symposium on ultrasound in schistosomiasis. Mem Inst Oswaldo Cruz 2001; 96:151-156.) with splenomegaly or previous history of splenectomy. All of these patients had a history of contact with contaminated water, a positive stool test for S. mansoni, or prior treatment for schistosomiasis.

The sample size was calculated using statistical software (EpiInfo version 3.5.5, Atlanta, U.S) to allow 80% power at a 5% significance level. Considering an expected frequency of PPF severity of 8% and a 4% margin of error with a 95% confidence level, the sample size was estimated to be 180 individuals⁷7. Henri S, Chevillard C, Mergani A, Paris P, Gaudart J, Camilla C, et al. Cytokine regulation of periportal fibrosis in humans infected with Schistosoma mansoni: IFN-gamma is associated with protection against fibrosis and TNF-alpha with aggravation of disease. J Immunol 2002; 169:929-936.,⁸8. Domingues AL, Lima AR, Dias HS, Leão GC, Coutinho A. Na ultrasonographic study of liver fibrosis in patients infected with Schistosoma mansoni in northeast Brazil. Trans R Soc Trop Med Hyg 1993; 87:555-558..

The variables related to risk factors for developing PPF were arranged in two groups: the socioeconomic and demographic variables, including gender, age, education level, family income, alcoholism, and site of contact with contaminated water; and the clinical variables, including history of severe gastrointestinal bleeding, hepatomegaly, splenomegaly, and specific treatment. The instrument used for investigating these factors was a pre-coded, structured questionnaire applied to individuals by a single operator.

Ultrasound evaluation

The diagnosis of the clinical form of disease was determined using the patient's clinical history and a clinical examination. An ultrasound evaluation of the upper abdomen was also performed by a single operator at the Gastrointestinal Endoscopy Unit of CH/UFPE using a Siemens Acuson X 150^® device with a 3.5-mHz convex transducer to confirm the diagnosis and rule out other liver diseases (Figure 2). The parameters used to define the PPF pattern were based on Niamey's classification¹⁴14. Richter J, Domingues AL, Barata CH, Prata AR, Lambertucci JR. Report of the second satellite symposium on ultrasound in schistosomiasis. Mem Inst Oswaldo Cruz 2001; 96:151-156.: C - peripheral; D - central; E - advanced; and F - very advanced.

FIGURE 2
Ultrasound features of periportal fibrosis patterns E (A) and D (B), according to Niamey's classification.

Statistical analysis

Data from the questionnaires were tabulated twice. Univariate and multivariate analyses were conducted using EpiInfo software version 3.5.5. For evaluating the association of selected factors and the fibrosis pattern, prevalence ratios (PRs) and 95% confidence intervals (CIs) were calculated using the fibrosis pattern as a dependent variable and the selected factors as independent variables. The potentially confounding variables with the factors of interest were examined using a non-conditional logistic regression analysis. The association was regarded as significant when p < 0.05.

Ethical considerations

All clinical and ultrasound examinations were performed according to a standardized protocol. The study was conducted within the standards required by the Declaration of Helsinki and was approved by the Research Ethics Committee of the Center for Health Sciences of Universidade Federal de Pernambuco under the Protocol 437/11.

RESULTS

The sample consisted of 178 individuals (Figure 1), 41.8% of which were male and 58.2% of which were female. The average age was 54 years and ranged from 18 to 89 years. The risk factors for developing PPF were illiteracy (PR 1.46, 95% CI 1 to 2.13, p = 0.026) and site of contact with contaminated water, particularly in the towns within the Metropolitan Region of Recife (PR 0.490, 95% CI 0.22 to 1.08, p = 0.014) and in the Zona da Mata of Pernambuco (PR 1.21, 95% CI 1.05 to 1.40, p = 0.029). The initial evaluations and tests of the associations between the explanatory variables and the PPF pattern are presented in Tables 1 and 2.

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TABLE 1
- Univariate analysis of the association between sociodemographic variables and the pattern of periportal fibrosis in Pernambuco, Brazil, 2012.

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TABLE 2
- Univariate analysis of the association between alcoholism, contact with contaminated water, specific treatment, and the periportal fibrosis pattern in Pernambuco, Brazil, 2012.

Clinical and ultrasound evaluation

Liver abnormalities were identified in 170 patients who were attributed to S. mansoni according to Niamey's protocol¹⁴14. Richter J, Domingues AL, Barata CH, Prata AR, Lambertucci JR. Report of the second satellite symposium on ultrasound in schistosomiasis. Mem Inst Oswaldo Cruz 2001; 96:151-156.. In the control group, there was PPF in the peripheral pattern in 11 (26.8%) individuals and in the central pattern in 22 (53.7%); 8 (19.5%) of these patients had no fibrosis. In the cases, the advanced pattern was detected in 110 (80.2%) cases, and the very advanced pattern was detected in 27 (19.8%) cases. With regard to the clinical variables, among the HS individuals, 76 (55.4%) had episodes of severe gastrointestinal bleeding, 59 (43.1%) were splenectomized, and 83 (60.5%) showed no hepatomegaly on physical examination.

On multivariate analysis, there were inverse associations between education level (up to 11 years of study) and specific treatment with the advanced PPF pattern, indicating that these variables may be protective factors. Table 3 shows the odds ratios (ORs) associated with the variables that remained in the final logistic regression model. For the final analysis, we selected 9 variables (education, time of last contact with contaminated water, site of last contact with contaminated water, alcoholism, specific treatment for S. mansoni, family income, last specific treatment, age, and gender). This analysis was used to evaluate the association between the PPF pattern (dependent variable) and the selected variables (independent variables).

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TABLE 3
- Final multiple logistic regression model for the advanced periportal fibrosis pattern.

The variables with p < 0.20 in the univariate analysis were included in the logistic regression model. We had to exclude patients in both groups due to lack of information for this analysis. The exclusions occurred in the analysis of the variables ‘last time of specific treatment’ - 16 cases/10 controls; ‘specific treatment for S. mansoni’ - 5 cases/5 controls and ‘time of last contact with contaminated water’ - 2 cases.

DISCUSSION

Protective associations were identified between the education level up to 11 years of study and prior specific treatment and the advanced periportal fibrosis pattern.

It has been shown that specific treatment for S. mansoni can contribute to decreasing infection levels and improving clinical conditions such as hepatosplenomegaly and PPF¹⁵15. Domingues ALC. Diagnóstico por imagem. In: Carvalho OS, Coelho PMZ, Lenzi HL, editors. Schistosoma mansoni e esquistossomose:uma visão multidisciplinar. Rio de Janeiro: Editora Fiocruz; 2008. p.929-61.–¹⁷17. Voieta I, Queiroz LC, Andrade LM, Silva LCS, Fontes VF, Barbosa AJ, et al. Imaging techniques and histology in the evaluation of lver fibrosis in hepatoesplenic schistosomiasis mansoni in Brazil: a comparative study. Mem Inst Oswaldo Cruz 2010; 105:414-421.. As a result, the regression of PPF may prevent the emergence of portal hypertension, highlighting the importance of PPF diagnosis by obtaining accurate methods for monitoring this disease¹⁸18. Espirito Santo MCC, Azeredo LM, Teles HMS, Gryschek RCB, Ferreira CS, Amato Neto V. Abdominal ultrasound in the evaluation of fibrosis and portal hypertension in area of schistosomiasis low endemicity. Rev Inst Med Trop Sao Paulo 2008; 50:117-119.. However, a higher education level might lead the patient to seek early treatment and could prevent reinfections.

Ultrasound examination and Niamey's classification¹⁴14. Richter J, Domingues AL, Barata CH, Prata AR, Lambertucci JR. Report of the second satellite symposium on ultrasound in schistosomiasis. Mem Inst Oswaldo Cruz 2001; 96:151-156. were used to diagnose the clinical forms and the PPF stages, which are currently the most widely used techniques for this purpose in both field and hospital studies⁴4. Prata A, Ruiz-Guevara R, Antunes CMF, Marinho CC, Queiroz LC, Voieta I, et al. Comparação entre achados clínicos e ultrassonográficos no diagnóstico da fibrose periportal em uma área endêmica de esquistossomose no Brasil. Rev Soc Bras Med Trop 2010; 43:129-134..

This study was hospital-based; individuals generally present with more severe clinical forms in hospital studies when compared to field studies. There were many HS schistosomiasis patients with advanced fibrosis and even HI individuals presenting the more advanced fibrosis pattern D when compared to pattern C. Only 8 individuals did not exhibit fibrosis. In an area with a low prevalence of this disease, most of the population did not show fibrosis, and only 4.6% had fibrosis pattern C¹⁸18. Espirito Santo MCC, Azeredo LM, Teles HMS, Gryschek RCB, Ferreira CS, Amato Neto V. Abdominal ultrasound in the evaluation of fibrosis and portal hypertension in area of schistosomiasis low endemicity. Rev Inst Med Trop Sao Paulo 2008; 50:117-119..

We observed an improvement in the education level in the patients from rural areas compared with previous studies, possibly due to Brazilian socioeconomic growth in recent years¹⁹19. Silva PCV, Domingues ALC. Aspectos epidemiológicos da esquistossomose hepatoesplênica no estado de Pernambuco, Brasil. Epidemiol Serv Saude 2011; 20:327-336.,²⁰20. Barbosa CS, Barbosa FS. Padrão epidemiológico da esquistossomose em comunidade de pequenos produtores rurais de Pernambuco, Brasil. Cad Saude Publica 1998; 14:129-137.. It is well known that control measures such as sanitation and education are gradually improving in Brazil; these measures contribute to a decrease in schistosomiasis transmission. In addition, better economic conditions for all individuals in northeastern Brazil may help to solve this public health problem, which still affects many states in the region, particularly Pernambuco¹⁹19. Silva PCV, Domingues ALC. Aspectos epidemiológicos da esquistossomose hepatoesplênica no estado de Pernambuco, Brasil. Epidemiol Serv Saude 2011; 20:327-336.,²¹21. Resendes APC, Souza SR, Barbosa CS. Hospitalization and mortality from mansoni schistosomiasis in the state of Pernambuco, Brazil, 1992/2000. Cad Saude Publica 2005; 21:1392-1401.,²²22. Barbosa CS, Araújo KC, Sevilla MAA, Melo F, Gomes ECS, Santos RS. Current epidemiological status of schistosomiasis in the state of Pernambuco, Brazil. Mem Inst Oswaldo Cruz 2010; 105:549-554.. In addition, studies have described recent transmissions of schistosomiasis throughout this region and even in the City of Recife¹⁹19. Silva PCV, Domingues ALC. Aspectos epidemiológicos da esquistossomose hepatoesplênica no estado de Pernambuco, Brasil. Epidemiol Serv Saude 2011; 20:327-336..

This study demonstrated that the prevailing sites with severe forms of schistosomiasis are still within the Zona da Mata of Pernambuco by evaluating the towns with higher frequencies of contact with contaminated water, although there has been an expansion of the disease to urban areas, especially within the Metropolitan Region of Recife and near the coast. The development of the severe form requires a high parasitic load, which means that the individual has undergone repeated contact with the infection focus over a long time. This is more frequently observed in the Zona da Mata than in the current foci in the metropolitan region of Recife and the coast of Pernambuco. Contact with these more recent foci is less intense. Moreover, it has been shown that HS schistosomiasis needs 5 to 15 years for the infection to establish itself²³23. Prata AR, Bina JC. Development of the hepatoesplenic form schistosomias. Gaz Med Bahia 1968; 68:49-60..

The high (55.4%) frequencies of gastrointestinal bleeding and prior splenectomy (43.1%) for the treatment of portal hypertension in these patients and the significant percentage of patients with no prior treatment (30.7%) reinforce the need for a systematic approach to the specific treatment of all cases with a positive diagnosis, particularly those with a diagnosis of the hepatosplenic form with advanced PPF. Evaluation and monitoring of esophageal varices and improvements in hospitals located in endemic areas to provide emergency care for HS schistosomiasis patients are needed to decrease the morbidity and mortality of this parasitic disease.

In conclusion, the risk factors evaluated in this study reinforce the impact of this disease in endemic areas of the State of Pernambuco, once again drawing attention to the fact that treatment and education constitute preventive factors for this disease. These data also indicate the need to implement social, sanitary, and health education interventions aimed at schistosomiasis to decrease or prevent disease occurrence, which is still a major public health problem.

REFERENCES

¹
World Health Organization (WHO). Programs and projects: schistosomiaisis. A major public health. 2010. [Cited 2010 February 25]. Available at: http://www.who.int/schistosomiaisis/en/
»
²
Amaral RS, Tauil PL, Lima DD, Engels D. An analysis of the impact of the schistosomiasis control programme in Brazil. Mem Inst Oswaldo Cruz 2006; 101:79-85.
³
Katz N, Peixoto SV. Análise crítica da estimativa do número de portadores de esquistossomose mansoni no Brasil. Rev Soc Bras Med Trop 2000; 33:303-308.
⁴
Prata A, Ruiz-Guevara R, Antunes CMF, Marinho CC, Queiroz LC, Voieta I, et al. Comparação entre achados clínicos e ultrassonográficos no diagnóstico da fibrose periportal em uma área endêmica de esquistossomose no Brasil. Rev Soc Bras Med Trop 2010; 43:129-134.
⁵
Abath FGC, Morais CNL, Montenegro CEL, Wynn TA, Montenegro SML. Immunopathogenic mechanisms in schistosomiasis: what can be learnt from human studies? Trends Parasitol 2006; 22:85-91.
⁶
Andrade ZA. Schistosomiasis and liver fibrosis. Parasite Immunology 2009, 31:656-663.
⁷
Henri S, Chevillard C, Mergani A, Paris P, Gaudart J, Camilla C, et al. Cytokine regulation of periportal fibrosis in humans infected with Schistosoma mansoni: IFN-gamma is associated with protection against fibrosis and TNF-alpha with aggravation of disease. J Immunol 2002; 169:929-936.
⁸
Domingues AL, Lima AR, Dias HS, Leão GC, Coutinho A. Na ultrasonographic study of liver fibrosis in patients infected with Schistosoma mansoni in northeast Brazil. Trans R Soc Trop Med Hyg 1993; 87:555-558.
⁹
Araujo KCGM, Resendes APC, Souza-Santos R, Silveira Júnior JC, Barbosa CS. Análise espacial dos focos de Biomphalaria glabrata e de casos humanos de esquistossomose mansônica em Porto de Galinhas, Pernambuco, Brasil, no ano 2000. Cad Saude Publica 2007; 23:409-417.
¹⁰
Pordeus LC, Aguiar LR, Quinino LRM, Barbosa CS. A ocorrência das formas aguda e crônica da esquistossomose mansônica no Brasil no período de 1997 a 2006: uma revisão de literatura. Epidemiol Serv Saude 2008,17:163-175.
¹¹
Dessein A, Chevillard C, Arnaud V, Hou X, Hamdoun AA, Dessein H, et al. Variants of CTGF are associated with hepatic fibrosis in chinese, sudanese, and brazilians infected with schistosomes. J Exp Med 2009; 12:1-8.
¹²
Brandt CT, Rino M, Pitta MGR, Muniz JS, Silveira DO, Castro CMMB. Avaliação das citocinas Il-10 e Il-13 como mediadores na progressão da fibrose de symmers em portadores de esquistossomose mansônica na forma hepatoesplênica. Rev Col Bras Cir 2010; 37:333-337.
¹³
Joshi VA, Roberts AE, Kucherlapati R. Towards a Treatment for RAS-MAPK pathway disorders. In: Zenker M, editor. Syndrome and related disorders: A matter of deregulated ras signaling. Monographs in human genetics: Basel Karger; 2008. p. 151-164.
¹⁴
Richter J, Domingues AL, Barata CH, Prata AR, Lambertucci JR. Report of the second satellite symposium on ultrasound in schistosomiasis. Mem Inst Oswaldo Cruz 2001; 96:151-156.
¹⁵
Domingues ALC. Diagnóstico por imagem. In: Carvalho OS, Coelho PMZ, Lenzi HL, editors. Schistosoma mansoni e esquistossomose:uma visão multidisciplinar. Rio de Janeiro: Editora Fiocruz; 2008. p.929-61.
¹⁶
Coutinho A, Domingues ALC. Specific Treatment of advanced schistosomiasis liver disease in man: favourable results. Mem Inst Oswaldo Cruz 1987; 82:335-340.
¹⁷
Voieta I, Queiroz LC, Andrade LM, Silva LCS, Fontes VF, Barbosa AJ, et al. Imaging techniques and histology in the evaluation of lver fibrosis in hepatoesplenic schistosomiasis mansoni in Brazil: a comparative study. Mem Inst Oswaldo Cruz 2010; 105:414-421.
¹⁸
Espirito Santo MCC, Azeredo LM, Teles HMS, Gryschek RCB, Ferreira CS, Amato Neto V. Abdominal ultrasound in the evaluation of fibrosis and portal hypertension in area of schistosomiasis low endemicity. Rev Inst Med Trop Sao Paulo 2008; 50:117-119.
¹⁹
Silva PCV, Domingues ALC. Aspectos epidemiológicos da esquistossomose hepatoesplênica no estado de Pernambuco, Brasil. Epidemiol Serv Saude 2011; 20:327-336.
²⁰
Barbosa CS, Barbosa FS. Padrão epidemiológico da esquistossomose em comunidade de pequenos produtores rurais de Pernambuco, Brasil. Cad Saude Publica 1998; 14:129-137.
²¹
Resendes APC, Souza SR, Barbosa CS. Hospitalization and mortality from mansoni schistosomiasis in the state of Pernambuco, Brazil, 1992/2000. Cad Saude Publica 2005; 21:1392-1401.
²²
Barbosa CS, Araújo KC, Sevilla MAA, Melo F, Gomes ECS, Santos RS. Current epidemiological status of schistosomiasis in the state of Pernambuco, Brazil. Mem Inst Oswaldo Cruz 2010; 105:549-554.
²³
Prata AR, Bina JC. Development of the hepatoesplenic form schistosomias. Gaz Med Bahia 1968; 68:49-60.

CONFLICT OF INTEREST: The authors declare that there is no conflict of interest.

FINANCIAL SUPPORT: Universidade Federal de Pernambuco (UFPE), Brazil.

Publication Dates

Publication in this collection
Jul-Aug 2013

History

Received
22 May 2013
Accepted
23 July 2013

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] ¹
World Health Organization (WHO). Programs and projects: schistosomiaisis. A major public health. 2010. [Cited 2010 February 25]. Available at: http://www.who.int/schistosomiaisis/en/
»

[2] ²
Amaral RS, Tauil PL, Lima DD, Engels D. An analysis of the impact of the schistosomiasis control programme in Brazil. Mem Inst Oswaldo Cruz 2006; 101:79-85.

[3] ³
Katz N, Peixoto SV. Análise crítica da estimativa do número de portadores de esquistossomose mansoni no Brasil. Rev Soc Bras Med Trop 2000; 33:303-308.

[4] ⁴
Prata A, Ruiz-Guevara R, Antunes CMF, Marinho CC, Queiroz LC, Voieta I, et al. Comparação entre achados clínicos e ultrassonográficos no diagnóstico da fibrose periportal em uma área endêmica de esquistossomose no Brasil. Rev Soc Bras Med Trop 2010; 43:129-134.

[5] ⁵
Abath FGC, Morais CNL, Montenegro CEL, Wynn TA, Montenegro SML. Immunopathogenic mechanisms in schistosomiasis: what can be learnt from human studies? Trends Parasitol 2006; 22:85-91.

[6] ⁶
Andrade ZA. Schistosomiasis and liver fibrosis. Parasite Immunology 2009, 31:656-663.

[7] ⁷
Henri S, Chevillard C, Mergani A, Paris P, Gaudart J, Camilla C, et al. Cytokine regulation of periportal fibrosis in humans infected with Schistosoma mansoni: IFN-gamma is associated with protection against fibrosis and TNF-alpha with aggravation of disease. J Immunol 2002; 169:929-936.

[8] ⁸
Domingues AL, Lima AR, Dias HS, Leão GC, Coutinho A. Na ultrasonographic study of liver fibrosis in patients infected with Schistosoma mansoni in northeast Brazil. Trans R Soc Trop Med Hyg 1993; 87:555-558.

[9] ⁹
Araujo KCGM, Resendes APC, Souza-Santos R, Silveira Júnior JC, Barbosa CS. Análise espacial dos focos de Biomphalaria glabrata e de casos humanos de esquistossomose mansônica em Porto de Galinhas, Pernambuco, Brasil, no ano 2000. Cad Saude Publica 2007; 23:409-417.

[10] ¹⁰
Pordeus LC, Aguiar LR, Quinino LRM, Barbosa CS. A ocorrência das formas aguda e crônica da esquistossomose mansônica no Brasil no período de 1997 a 2006: uma revisão de literatura. Epidemiol Serv Saude 2008,17:163-175.

[11] ¹¹
Dessein A, Chevillard C, Arnaud V, Hou X, Hamdoun AA, Dessein H, et al. Variants of CTGF are associated with hepatic fibrosis in chinese, sudanese, and brazilians infected with schistosomes. J Exp Med 2009; 12:1-8.

[12] ¹²
Brandt CT, Rino M, Pitta MGR, Muniz JS, Silveira DO, Castro CMMB. Avaliação das citocinas Il-10 e Il-13 como mediadores na progressão da fibrose de symmers em portadores de esquistossomose mansônica na forma hepatoesplênica. Rev Col Bras Cir 2010; 37:333-337.

[13] ¹³
Joshi VA, Roberts AE, Kucherlapati R. Towards a Treatment for RAS-MAPK pathway disorders. In: Zenker M, editor. Syndrome and related disorders: A matter of deregulated ras signaling. Monographs in human genetics: Basel Karger; 2008. p. 151-164.

[14] ¹⁴
Richter J, Domingues AL, Barata CH, Prata AR, Lambertucci JR. Report of the second satellite symposium on ultrasound in schistosomiasis. Mem Inst Oswaldo Cruz 2001; 96:151-156.

[15] ¹⁵
Domingues ALC. Diagnóstico por imagem. In: Carvalho OS, Coelho PMZ, Lenzi HL, editors. Schistosoma mansoni e esquistossomose:uma visão multidisciplinar. Rio de Janeiro: Editora Fiocruz; 2008. p.929-61.

[16] ¹⁶
Coutinho A, Domingues ALC. Specific Treatment of advanced schistosomiasis liver disease in man: favourable results. Mem Inst Oswaldo Cruz 1987; 82:335-340.

[17] ¹⁷
Voieta I, Queiroz LC, Andrade LM, Silva LCS, Fontes VF, Barbosa AJ, et al. Imaging techniques and histology in the evaluation of lver fibrosis in hepatoesplenic schistosomiasis mansoni in Brazil: a comparative study. Mem Inst Oswaldo Cruz 2010; 105:414-421.

[18] ¹⁸
Espirito Santo MCC, Azeredo LM, Teles HMS, Gryschek RCB, Ferreira CS, Amato Neto V. Abdominal ultrasound in the evaluation of fibrosis and portal hypertension in area of schistosomiasis low endemicity. Rev Inst Med Trop Sao Paulo 2008; 50:117-119.

[19] ¹⁹
Silva PCV, Domingues ALC. Aspectos epidemiológicos da esquistossomose hepatoesplênica no estado de Pernambuco, Brasil. Epidemiol Serv Saude 2011; 20:327-336.

[20] ²⁰
Barbosa CS, Barbosa FS. Padrão epidemiológico da esquistossomose em comunidade de pequenos produtores rurais de Pernambuco, Brasil. Cad Saude Publica 1998; 14:129-137.

[21] ²¹
Resendes APC, Souza SR, Barbosa CS. Hospitalization and mortality from mansoni schistosomiasis in the state of Pernambuco, Brazil, 1992/2000. Cad Saude Publica 2005; 21:1392-1401.

[22] ²²
Barbosa CS, Araújo KC, Sevilla MAA, Melo F, Gomes ECS, Santos RS. Current epidemiological status of schistosomiasis in the state of Pernambuco, Brazil. Mem Inst Oswaldo Cruz 2010; 105:549-554.

[23] ²³
Prata AR, Bina JC. Development of the hepatoesplenic form schistosomias. Gaz Med Bahia 1968; 68:49-60.

Characteristics	Periportal fibrosis groups				PR	95%CI	p-value^* * χ2 : chi-square.
	Grupo 1		Group 2
	n	%	n	%
Gender
male	58	42.3	16	39.0	1.03	0.88-1.21	0.8439
female	79	57.7	25	61.0
total	137	100.0	41	100.0
Age (years)
18 to 40	22	16.0	8	19.5	1	0.76-1.30	0.825
41 to 60	73	53.2	18	44.0	1.09	0.90-1.31	0.467
≥ 61	42	30.6	15	36.5	1
total	137	100.0	41	100.0
Education
illiteracy	28	20.4	4	9.7	1.46	1-2.13	0.026
1 to 8 years	97	70.8	29	70.7	1.28	0.89-1.86	0.178
9 to 11 years	12	8.7	8	19.5	1
total	137	100.0	41	100.0
Family income
< 1 minimum wage	21	15.3	2	4.9	1.17	0.81-1.70	0.556
1 to 3 minimum wages	109	79.5	37	90.2	0.96	0.67-1.38	0.596
≥ 4 minimum wages	7	5.1	2	4.9	1
total	137	100.0	41	100.0

Variables	Periportal fibrosis groups				PR	95%CI	p-value^* * χ2 : chi-square.
	Grupo 1		Group 2
	n	%	n	%
Alcoholism
yes	12	8.7	6	14.6	0.85	0.61-1.20	0.207
no	125	91.3	35	85.3
total	137	100.0	41	100.0
CCW
MRR	4	2.9	7	17.0	0.49	0.22-1.08	0.014
Zona da Mata	53	38.6	6	14.6	1.21	1.05-1.40	0.029
Coast	5	3.6	2	4.8	0.96	0.59-1.56	0.584
others	75	54.7	26	63.4	1
total	137	100.0	41	100.0
Last exposure time^* * χ2 : chi-square.
≤ 1 year	15	11.2	1	2.4	1
≥ 1 to 15 years	41	30.4	14	34.1	0.80	0.65-0.97	0.089
> 15 to 25 years	26	19.2	10	24.3	0.77	0.61-0.98	0.077
≥ 25 years	53	39.2	16	39.0	0.82	0.68-0.98	0.114
total	135	100.0	41	100.0
Specific treatment^ 10 patients (5 cases/5 controls) with no information were excluded;
oxamniquine	09	6.9	2	5.5	1
praziquantel	112	84.8	26	72.2	0.99	0.74-1.33	0.658
did not undergo	11	8.5	8	22.2	0.71	0.44-1.14	0.175
total	132	100.0	36	100.0
Last treatment^* ***** 26 patients (16 cases/10 controls) with no information were excluded;
≤ 1 year	32	26.4	10	32.2	1
≥ 1 to 15 years	83	68.5	19	61.2	1.07	0.88-1.30	0.633
≥ 15 to 25 years	6	5.0	2	6.4	0.98	0.64-1.52	0.626
total	121	100.0	31	100.0

Variables	Adjusted OR^* * χ2 : chi-square.	95% CI	p-value
Education
illiteracy	1
≥ 11 years	0.7198	0.5491-0.9434	0.0172
Treatment for SM
treated (PZ/OX)	0.7612	0.5819-0.9956	0.0464
not treated	1

Brasil

Brasil

Treatment and education reduce the severity of schistosomiasis periportal fibrosis

Abstract

Introduction

Methods

Results

Conclusions

INTRODUCTION

METHODS

Selection of patients

Ultrasound evaluation

Statistical analysis

Ethical considerations

RESULTS

Clinical and ultrasound evaluation

DISCUSSION

REFERENCES

Publication Dates

History