Schistosomiasis: Review of an immune complex disease

EO Yusuf and Lucy U. Airauhi

ABSTRACT
BACKGROUND: Morbidity due to human schistosomiasis is associated with host immune responses which result in immune based inflammation, granuloma formation and fibrotic lesions.

MATERIALS AND METHODS: This is a review of the literature on the immunology of schistosomiasis and the description of the immunopathogenesis of the disease. Relevant articles were retrieved using electronic search and hand search of published literature.

RESULTS: Host responses which include immune based inflammation, granuloma formation and fibrotic lesions are aimed at destroying schistosome ova lodged in the liver, intestinal and bladder walls, and other tissues. At the site of the infection, ‘swimmers’ itch is due to physical damage to the skin by proteases and other toxic substances secreted by cercaria. During intestinal Schistosomiasis, the parasitic ova are lodged in the liver provoking fibrogenesis, while during urinary schistosomiasis pathology is attributed to the formation of granuloma along the urinary tract, there is fibrosis which lead to strictures, calcification and urodynamic abnormalities. The classic descriptions of schistosomiasis-related morbidity focus on pathologies unique to schistosome infection: periportal fibrosis for intestinal schistosomiasis and bladder deformity and hydronephrosis for urogenital schistosomiasis.

CONCLUSION: This review provides some useful information concerning some aspects of the relationships between Schistosoma species and the human host.

INTRODUCTION
Schistosomiasis is a cause of significant parasitic morbidity and mortality in endemic countries. It is also known as bilharziasis after Theodor Bilharz who discovered the causative agent in Egypt in 1851. The disease has a relatively low mortality but high morbidity; causing severe debilitating illness in millions of people. It is caused by an infection with Schistosoma species of helminthic flat worms known as flukes belonging to the class Trematoda of the phylum Platyhelminthes.1 The parasite afflict at least 243 million people.2,3
Most infections are subclinical but may progress to chronic forms characterized by the presence of liver, intestinal and kidney involvement.4
Schistosoma parasites display considerable biodiversity in habitat5 there are two major forms of schistosomiasis: intestinal caused by four main species S.mansoni, S.japonicum, S. mekongi, S. guineensis and S. intercalatum while urogenital form of the disease is caused by S. haematobium.1,4

METHODS
Information for this review were from the comprehensive search of titles related to the immunology of schistosomiasis using PUBMED and other bibliographic data bases between 1985 and 2016 using key words, immunology, immunopathogenesis, epidemiologic trends and pathology of schistosomiasis. Relevant websites such as that of the World Health Organization (WHO) were also searched.

LIFE CYCLE
Infection is initiated by the infectious cercariae which burrow into the skin, transform into schistosomulae and then enter the vasculature, migrate to the portal system where they cross the endothelium and basement membrane of the vein and traverse the intervening tissue, basement membrane and epithelium of the intestine (S. mansoni, S. japonicum and other associated species) or bladder (S. haematobium). Adult male and female worms mate and produce fertilized eggs in the veins of their human hosts where they live for an average of between 3-19 years, with longevity records that extend for several decades.6,7
After a period of about 5-7 weeks the parasite matures to egg producing worms8 and excretion to the exterior begins, the eggs hatch in water releasing free living ciliated miracidium9; suitable snail hosts are then infected by cercariae where asexual reproduction occurs through mother and daughter sporocyst producing thousands of cercariae which are infectious for humans.
The worms live within the perivesical (S. haematobium) or mesenteric (S.mansoni; S.japonicum and others) venules; they digest erythrocytes obtaining energy by glucose metabolism.10,11
The clinical features of human schistosomiasis depend on the species, developmental stage, and site of infection in the body. It comprises three major syndromes: cercarial dermatitis, acute schistosomiasis or katayama fever and chronic fibro-obstructive disease.4

Epidemiology
Schistosomiasis is an acute and chronic disease caused by parasitic worms of the genus Schistosoma.1
There are two major forms of schistosomiasis: intestinal and urogenital; two hosts are required for the parasite to complete its life cycle (a vertebrate and a snail host). Snails of the genera Biomphalaria, Bulinus, Neotricula and Onchomelania are the principal intermediate hosts for S. mansoni, S. haematobium, S. mekongi and S.japonicum respectively.2,5
The intermediate hosts are more abundant during dry season in the tropics when temperatures are as high as between 480-500C; and children often go to the streams to reduce the heat of the day and for recreation12; this exposes them to infection. People are infected during routine agricultural, domestic and recreational activities which expose them to infection.13
The disease is prevalent in tropical and subtropical areas especially poor communities without access to safe drinking water and adequate sanitation.1
Transmission occurs when infected people contaminate fresh water with their excreta or urine which contains the eggs of the parasite. The eggs hatch releasing miracidia which infect appropriate snail hosts to continue their life cycle. Asexual reproduction occurs with the emergence of infectious cercariae. Following skin penetration by cercariae, they migrate in the circulation to the liver, develop into male or female, pair up and home to appropriate habitats.
There is no sex predilection to infection both sexes are equally susceptible to schistosomiasis; different local, cultural and social practices may predispose either sex to higher infection.

Immunopathogenesis
The mechanism of pathogenicity of Schistosoma is attributable to the antigenic secretions of the parasites which perturbs the immune system of the host; including type I and type IV hypersensitivity reactions.14
Life cycle stages of the parasite express several antigens that the host immune system confront15,16 the challenges posed stimulate humoral and cellular responses. The life cycle stages which express antigens include juvenile worms, adult worm and egg: penetrating cercariae, migrating schistosomulae, adult worm and eggs produced by the adult worm.15,16
There is an overriding differential pattern in the host's immune responses against worm-derived antigens when compared to egg derived antigen.17 This is seen as early high level responses to soluble egg antigen (SEA) that decreases as infection becomes chronic.18,19,20
However responses to soluble worm antigen preparations (SWAP) rises early in the course of infection and continues to be expressed throughout the chronic stage of infection.21
During infection with any Schistosoma species, chronic disease is the result of the ongoing host response to accumulating tissue-trapped eggs.
In, S. mansoni and S. japonicum infections, the liver is the principal site that is affected because, many of the eggs are carried by the blood into this organ and the sinusoids are too narrow for the eggs to traverse. This is a dead end for the eggs which eventually die within the tissue. Symmers' fibrosis of the liver which may result in portal hypertension and congestive splenomegaly is the most severe form of intestinal schistosomiasis.22
During S. haematobium infection, the passage of eggs across the bladder wall causes damage to the organ. The CD4+ T response that is induce by egg antigens orchestrates the development of granulomatous lesions which are composed of collagen fibers and cells which include macrophages, eosinophils and CD4+T cells around individual eggs.23
In intestinal schistosomiasis, eggs swept back to the liver in the portal circulation lead to chronic inflammation and fibrosis of the portal triad; eventually resulting in cirrhosis, portal hypertension, splenomegaly and bleeding esophageal varices.1
In genitourinary infections, the bladder, lower ureters, seminal vesicles are often involved, less frequently involved are: the vas deferens, prostate and female genital system.14
The initial lesions are mucosal granulomas which coalesce to form tubercles, nodules or masses which usually ulcerate. The characteristic clinical presentation is terminal hematuria, usually associated with increased frequency of micturition and dysuria1; recurrent bacterial urinary tract infection, obstruction of ureters with the development of hydroureter and hydronephrosis and ultimately renal failure. The bladder mucosa appears pale with granular patches known as 'sandy patches' which are characteristic of healed schistosomiasis.14
Schistosoma granuloma is the typical 'unit' of the cellular immune response to schistosomal infecton14 It is composed of different blood and tissue cells being recruited by specific chemo-attractants and serving specific function and; although this is cellular in nature, the role of antibodies and complement has been documented in experimental models for decades.24
Local tissue injury resulting from passage of parasite eggs through the walls of the intestine to the bowel lumen is associated with abdominal pain and bloody stool in intestinal schistosomiasis and; the passage of parasite eggs through the urinary bladder wall, to the bladder lumen resulting in bloody urine in genito-urinary schistosomiasis.1
Circulating immune complexes have been reported to be involved in the pathogenesis of human schistosomiasis).25 Granular basement membrane deposits, immunoglobulin, compliments and parasite antigens have been demonstrated in the renal glomeruli of patients with chronic schistosomiasis.24 Chronic schistosomiasis is the consequence of parasite eggs trapped in tissues, with resulting granulomatous reaction to the eggs.1
Schistosoma parasites flourish in the human host despite the development of a pronounced immune response. This suggests that the immune response is incapable of preventing primary infection and; resistance to superinfection takes years to develop.26  It has been observed that the development of acquired immunity to human schistosomiasis is extremely slow;27,28 due to the following hypotheses: i) that dying worms are the main source of protective antigen which is delayed by the long parasite lifespan;29 ii) exposure to certain threshold level of antigen is required before protective response is stimulated.30 Despite the long time to taken to develop some degree of protective immunity, it rarely results in sterile immunity.27
In acute schistosomiasis, after initial infection with S.mansoni, S.japonicum or S. haematobium, a serious illness accompanied by high fever (Katayama fever) may be seen. This is due to the release of soluble parasite antigen into the circulation as the worms mature and begins to release eggs.1
Katayama fever is commonly associated with S.japonicum infection and is probably due to larger number of eggs released by the species. The onset of symptoms is about 20-40 days after exposure. This fever is less common in S.mansoni and rare with S. haematobium

CONCLUSION
This review is summary of the immunology of schistosomiasis which reflects the pathogenesis of the disease in humans. Host immune responses to the various developmental stages of the parasite produce cell mediated responses, granulomatous reaction and fibrosis.

REFERENCES:

  1. Jong EC. Schistosomiasis. Nettler’s Infectious Diseases.2013:516-512.
  2. Chitsulo L, LoVerck P and Engels D. Schistosomiasis. Nat, Rev. Microbiol 2004;2:12-13.
  3. World Health Organisation. Schistosomiasis Fact Sheet No 115. Available at:http://www.who.int/mediacentre/factsheets/fs115/en/(accessed 4 December 2013)
  4. WHO World report 2001.
  5. Kali A. Schistosome Infections: An Indian Perspective. Journal of Clinical and Diagnostic Research.2015;9(2): DE 01-DE02.doi10.7860/JCDR/2015/10512.553/
  6. Warren KS, Mahmoud AA, Cummings P, Murphy DJ, Houser HB. Schistosomiasis mansoni in Yemeni in California: duration of infection, presence of disease, therapeutic management. Am J. Trop Med Hyg.1974;23:902-909.
  7. Chabasse D, Bertrand G, Leroux JP, Gauthey N, Hocquet P. Developmental bilharziasis caused by Schistosoma mansoni discovered 37 years after infection. Bull Soc Pathol Exot.1985;78: 643-647
  8. Doenhoff MJ. A role for granulomatous inflammation in the transmission of infectious disease: schistosomiasis and tuberculosis. Parasitology. 1997; 115:113-125.
  9. Colley DG and Secor WE. Immunology of human schistosomiasis. Parasite Immunology 2014; 36: 347-357.
  10. Van Oordt BE, van den Heuvel JM, Tielens AG van den Bergh SG. The energy production of the adult Schistosoma mansoni is for a large part aerobic. Mol Biochem Parasitol 1985;16:117-126. Barret J. Forty years of helminth biochemistry. Parasitology 2009; 136: 1633-1642.
  11. Barrett J. Forty Years of Helminth Biochemistry. Parasitology. 2009; 136:1633-1642.
  12. Singh K, Muddasiru D and Singh J. Current Status of Schistosomiasis in Sokoto Nigeria. Parasite Epidemiology and Control. 2016; 1: 239-244.
  13. Yorsry A. Schistosomiasis and neoplasia. Contrib Microbiol 2006;13: 81-100.
  14. Barsoum RS  Urinary Schistosomiasis: Review. Journal of Advanced Research 2013:453-459.
  15. Verjovski-Almeida S, Leite LC, Dias-Neto E, Menck CF and Wilson RA. Schistosome  Transcritome: Ins sights and Perspectives for Functional Genomics: Trend Parasitol 2004;30: 304-308.
  16. Hokke CH, Fitzpatrick JM and Hoffman KF. Intergrating Transcriptome, Proteome and Glycome Analysis of Schistosoma Biology. Trends Parasitol 2007;23: 165-174.
  17. Williams ME, Montenegro ALS, Domingue. Leukocytes of Patients with Schistosoma mansoni respond with a Th2 Pattern of Cytokine Production to mitogen or egg antigens but with a Th0 pattern to worm antigens SG. Journal of infectious Diseases.1994;170(4):946-954.
  18. Colley DG, Cook JA, Freeman GL Jr, Bartholomew RK and Jordan P. Immune Responses during human schistosomiasis mansoni I In vitro lymphocyte blastogenic responses to heterogenous antigenic preparations from schistosome eggs, worms and cercariae. Int. Arch. Allergy Appl. Immunol. 1977;53: 420-433.
  19. Barsoum IS, Gamil FM, Al-Khalif MA, Ramzy RM, El ALamy MA and Colley DG. Immune responses  and immunoregulation in relation to human schistosomiasis in Egypt I. Effects of treatment on in vitro cellular responsiveness. Am J Trop Med Hyg 1982;31: 1181-1187
  20. Caldas IR, Campi-Azvedo AC, Oliveira RC and Gazzineli G. Human Schistosomiasis mansoni : immune responses during acute and chronic phases of infection. Acta Trop 2008;108:109-117.
  21. Naus CW, van Remootere A, Ouma JH et al. Specific antibody responses to three schistosome-related carbohydrate structures in recently exposed immigrants and established residents in an area of Schistosoma mansoni endemicity. Inect Immun 2003;71: 5676-5681. In: Colley DG and Secor WE. Immunology of human schistosomiasis. Parasite Immunology 2014;36: 347-357.
  22. Da Silva LC. Portal hypertension in schistosomiasis: Pathophysiology and Treatment.Mem.Inst Oswaldo Cruz, Rio de Janeiro 1992;87(suppl.iv):183-186.
  23. Dune DW and Pearce EJ. Immunology of hepatosplenic schistosomiasis mansoni: a human perspective . Microbes  Infect.1999.1:553-560.In: Pearce EJ and Mac Donald AS. The Immunology of schistosomiasis. Nature Review Immunology. 2002; 2:499-510.
  24. De Brito PA, Kazura JW, Mahmoud AA. Host granulomatous response in Schistosoma mansoni. Antibody and cell mediated damage of parasite egg in vitro.J. Clin Invest.1984;74(5): 1715-1723. In: Barsoum RS  Urinary Schistosomiasis: Reviw. Journal of Advanced Research 2013:453-459.
  25. Lawley TJ, Ottesen EA, Hiatt RA and Gazee LA.  Circulating immune      complexes in acute schistosomiasis. Clin exp. Immunol 1979; 37:221-227.
  26. Pearce EJ and Mac Donald AS. The Immunology of schistosomiasis. Nature Review Immunology. 2002; 2:499-510.
  27. Mutapi F, Billigsley PF and Secor WE. Infection and treatment immunisations for successful parasite vaccines. Trends Parasitol.2013;29: 135-141.
  28. Mitchel KM, Mustapi F, Savil NJ and Woolhouse MEJ. Protective immunity to Schistosoma haematobium infection is primarily an anti-fecundity response stimulated by death of worms. Proc Natl. Acad Sci.USA.2012;109(33):13347-13352.
  29. Woolhouse MEJ, Hagan P. Seeking the ghost of worms past. Nat Med 19995(11): 1225-1227.
  30. Mustapi F, Burchmore R, Mduluza T, Midzi N, Turner CM, Maizels RM. Age- related infection intensity-related shifts in antibody recognition of defined protein antigens in a schistosome-exposed population. J infect Dis.2008;198(2): 167-175.