Hyperreactive malarious splenomegaly and aids: a case report

Tano, Zuleica Naomi; Filho, Chafic Esper Kallas; Breganó, Regina Mitsuka; Pavanelli, Wander Rogério; Ruzon, Uheyna Gancedo

doi:10.1016/j.bjid.2014.04.005

Abstract

Malaria is endemic in the North of Brazil. However, Hyperreactive Malarious Splenomegaly (HMS) has been rarely described. Splenomegaly in HIV/Aids infection has a large differential diagnosis, but malaria is a cause of gross splenomegaly, regardless of the HIV status. In this paper, we report the case of a 50-year-old man, HIV positive, with massive splenomegaly and multiple malaria infections in the past. He fulfilled the criteria for HMS, received a short course of anti-malarial treatment and weekly quimioprofilatic Chloroquine. In 9 months, he had great clinical and laboratorial improvement confirming the HMS, a rare diagnosis in Brazil.

Hyperreactivemalarious; splenomegaly; Aids

Introduction

Hyperreactive malarious splenomegaly (HMS), known as Tropical Splenomegaly Syndrome,¹1. Bryceson A, Fakunle YM, Fleming AF, et al. Malaria and splenomegaly (letter). Trans R Soc Trop Med Hyg. 1983;77: 879. despite being common in malaria-endemic regions and in travelers from non-endemic areas,²2. Crane GG. Recent studies of hyperreactive malarious splenomegaly (tropical splenomegaly syndrome) in Papua New Guinea. P N G Med J. 1986;29:35-40. has low prevalence in Brazil.³3. Doenças Infecciosas e Parasitárias: Enfoque Amazônico/Raimundo Nonato Queiroz de Leão {coordenador}. Belém: Cejup, UEPA, Instituto Evandro Chagas; 1997. The HMS is presented as an exaggerated immune response to infection by Plasmodium, resulting in nonspecific, hyper-immunoglobulin M (IgM) polyclonal immunoglobulin production by B lymphocytes, and the formation of immune complexes that are deposited in the spleen. The criteria for the diagnosis of HMS are: splenomegaly (>10 cm below the left costal margin), increased IgM that exceeds twice the reference value, high titers of antibodies specific against Plasmodium sp. and clinical-laboratory improvement after treatment with anti-malarial drugs.⁴4. Fakunle YM. Tropical splenomegaly. Clin Hematol. 1981;10:963-75.,⁵5. Bates I, Bedu-Addo G. Review of diagnostic criteria of hyperreactive malarial splenomegaly. Lancet. 1997;349: 1179. The association with HIV infection is poorly documented, although HIV and malaria are endemic in many tropical regions.

Case report

A 50-year-old man was admitted to the infectious diseases sector of UHL (University Hospital of Londrina, Brazil) in February 2012. On admission, he complained of progressive weight loss, asthenia, and abdominal discomfort for two months, associated with fever for three days.

Physical examination showed discrete hepatomegaly and significant splenomegaly, about 20 cm below the left costal margin. He reported having lived in the cities of Londrina/PR and Itaituba/PA, where he worked in mining for about seven months a year. He had a previous history of 20 episodes of malaria, and had been diagnosed with HIV in the past two years, with irregular use of antiretroviral therapy. Laboratory tests on admission showed: Hb = 5.6 g/dL, platelets = 61,000/mm³; leukocytes = 4300/mm³ (67% neutrophils), protein electrophoresis with hypergamma-globulinemia = 51%; albumin = 2.5 g/dL; IgM = 1790mg/dL (NR: 57–212), CD4 = 115/mm³ and viral load = 2352 copies/mL. Antibody (indirect immunofluorescence) anti-plasmodium vivax was 1/1280 and anti-plasmodium falciparum = 1/320. The direct method for Plasmodium sp. thick smear was negative, as well as polymerase chain reaction (PCR). On admission, the first diagnostic hypothesis was sepsis after urinary tract infection. Once E. coli bacteria were isolated from blood and urine, the treatment with Ciprofloxacin had good response, but the urinary infection could not explain the splenomegaly.

Mieloculture was performed and fungi and Leishmania in two samples were searched, both turned out negative, ruling out histoplasmosis and visceral leishmaniasis. Inoculation in mice bone marrow blood resulted negative for Leishmania. Parasitical exams were negative in feces.

On admission, serology for toxoplasmosis and cytomegalovirus had positive IgM for both microorganisms, which ultimately proved to be false-positive. Likewise, anti-HCV was positive at low titers, with negative PCR for HCV.

Abdominal tomography showed a 3700 mL spleen at admission and 9 months after initiation of treatment, it reduced to 1358 mL (64% reduction), demonstrating homogeneous parenchymal liver and spleen without portal hypertension (Figs. 1 and 2).

Fig. 1
CT abdomen at admission.

Fig. 2
CT abdomen nine months after chloroquine use.

Having defined the diagnosis of HMS the first cycle with primaquine and chloroquine was carried out for 7 days, followed by chloroquine 300 mg/week. Follow-up exams in the first and ninth month are shown in Table 1.

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Table 1
Laboratory tests.

Discussion and conclusion

The development of HMS is associated with two main factors: repeated exposure to Plasmodium species and genetic predisposition. Countries with high endemism for malaria have prevalence of HMS ranging from 1 to 2% in Nigeria and 80% in certain tribes of New Papua Guinea.²2. Crane GG. Recent studies of hyperreactive malarious splenomegaly (tropical splenomegaly syndrome) in Papua New Guinea. P N G Med J. 1986;29:35-40.In Brazil, the prevalence is low in the Amazon region.³3. Doenças Infecciosas e Parasitárias: Enfoque Amazônico/Raimundo Nonato Queiroz de Leão {coordenador}. Belém: Cejup, UEPA, Instituto Evandro Chagas; 1997. Alecrim⁶6. Alecrim, WD. Estudo clínico e epidemiológico da malária no Rio Ituxi-Amazonas. 1979. 115p. Tese (mestrado). Universidade de Brasiília, Brasília. 1979. examined a population of 890 people living in a hyper-endemic area of Manaus, and found only 10 people with a persistent spleen enlargement. Of these, four met the criteria for Tropical Splenomegaly, as it was known at the time, three of them were brothers, underscoring the importance of genetic predisposition in tribal HMS.

The main genetic factors related to high population prevalence of HMS were HLA-DR2 and high levels of HLA heterozygous,⁴4. Fakunle YM. Tropical splenomegaly. Clin Hematol. 1981;10:963-75.,⁷7. Bhatia KK, Crane GG. HLA heterozygosity and hyperreactive malarious splenomegaly in the Upper Watut Valley of Nova Guinéa. P N G Med J. 1989;32:277-86. in addition to the high frequency of the haplotype IGHG3.⁸8. Kelly KM. IGHG3 G and the pathogenesis of hyperreactive malarious splenomegaly. Med Hypotheses. 1996;46:135-9.

It is believed that patients with HMS have a hyper production of polyclonal IgM,¹1. Bryceson A, Fakunle YM, Fleming AF, et al. Malaria and splenomegaly (letter). Trans R Soc Trop Med Hyg. 1983;77: 879. which is linked to suppressor T lymphocytes (cytotoxic phenotype), causing the elimination of the parasite, as well as generating immune complexes that are deposited in the spleen, thus resulting in splenomegaly.

In this case, the overproduction of nonspecific polyclonal IgM explains the false positive results for both cytomegalovirus and toxoplasmosis, in addition to high titers of IgM (one of the diagnostic criteria).

The diagnosis of tropical splenomegaly syndrome requires exclusion of other causes of massive splenomegaly. However, definite diagnosis depends on specific criteria, such as the Fakunle⁴4. Fakunle YM. Tropical splenomegaly. Clin Hematol. 1981;10:963-75.,⁵5. Bates I, Bedu-Addo G. Review of diagnostic criteria of hyperreactive malarial splenomegaly. Lancet. 1997;349: 1179.,⁹9. Ranjan K, Singh. Hyperreactive malarial splenomegaly in expatriates. Travel Med Infect Dis. 2007;5:24-9. criteria shown in Table 2. These criteria are not different for HIV patients.¹⁰10. De Iaco G, Saleri N, Perandin F, et al. Case Report. Hyper-reactive malarial splenomegaly in a patient with human immunodeficiency virus. Am J Trop Med Hyg. 2008;78:239-40. In the case herein reported, the patient met all major criteria in addition to hypersplenism as a minor criterion, thus confirming the diagnosis.

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Table 2
Diagnostic feature of hyperreactive malarious splenomegaly (HMS) - Fakunle criteria.

Although HIV/AIDS and malaria coexist with high prevalence in many countries of sub-Saharan Africa, few cases have been published linking the two diseases.¹⁰10. De Iaco G, Saleri N, Perandin F, et al. Case Report. Hyper-reactive malarial splenomegaly in a patient with human immunodeficiency virus. Am J Trop Med Hyg. 2008;78:239-40.,¹¹11. Lowenthal MN, Horowitz J, Gaspar N, et al. Hyperreactive malarial splenomegaly and AIDS: proguanil prevents recurrent pneumonia. Trans R Soc Trop Med Hyg. 1996;90:313-4. In individuals with AIDS there is an inversion in the CD4/CD8 ratio due to decrease in number and function of CD4T lymphocytes, while in HMS there is an increase in this ratio due to decreased number of CD8T lymphocytes. One hypothesis is that this difference may prevent patients with HIV from manifesting HMS after repeated Malaria infections, explaining therefore the low number of cases associating the two diseases. However, further studies should be carried out to better identify the immunological relationship between them.

HMS treatment consists of a short cycle of anti-malarial drug, and the use of chemoprophylaxis (chloroquine in this case) for a period of 9–26 months in patients who remain exposed to malaria, to prevent new infections and to have the described immunomodulatory effect of chloroquine.¹²12. Hoffman SL, Piessens WF, Ratiwayanto S, et al. Reduction of suppressor T lymphocytes in the tropical splenomegaly syndrome. N Engl J Med. 1984;310:337-41.

Therefore, we must be alert to cases of massive splenomegaly in patients living in endemic areas of malaria in Brazil, or those who migrated from these regions. Furthermore, HMS needs to be considered as a differential diagnosis in patients with splenomegaly and AIDS.

Acknowledgement

We would like to thank André Machado Siqueira from Univer-sidade Estadual do Amazonas (Amazonas State University) for the suport in malaria PCR.

REFERENCES

¹
Bryceson A, Fakunle YM, Fleming AF, et al. Malaria and splenomegaly (letter). Trans R Soc Trop Med Hyg. 1983;77: 879.
²
Crane GG. Recent studies of hyperreactive malarious splenomegaly (tropical splenomegaly syndrome) in Papua New Guinea. P N G Med J. 1986;29:35-40.
³
Doenças Infecciosas e Parasitárias: Enfoque Amazônico/Raimundo Nonato Queiroz de Leão {coordenador}. Belém: Cejup, UEPA, Instituto Evandro Chagas; 1997.
⁴
Fakunle YM. Tropical splenomegaly. Clin Hematol. 1981;10:963-75.
⁵
Bates I, Bedu-Addo G. Review of diagnostic criteria of hyperreactive malarial splenomegaly. Lancet. 1997;349: 1179.
⁶
Alecrim, WD. Estudo clínico e epidemiológico da malária no Rio Ituxi-Amazonas. 1979. 115p. Tese (mestrado). Universidade de Brasiília, Brasília. 1979.
⁷
Bhatia KK, Crane GG. HLA heterozygosity and hyperreactive malarious splenomegaly in the Upper Watut Valley of Nova Guinéa. P N G Med J. 1989;32:277-86.
⁸
Kelly KM. IGHG3 G and the pathogenesis of hyperreactive malarious splenomegaly. Med Hypotheses. 1996;46:135-9.
⁹
Ranjan K, Singh. Hyperreactive malarial splenomegaly in expatriates. Travel Med Infect Dis. 2007;5:24-9.
¹⁰
De Iaco G, Saleri N, Perandin F, et al. Case Report. Hyper-reactive malarial splenomegaly in a patient with human immunodeficiency virus. Am J Trop Med Hyg. 2008;78:239-40.
¹¹
Lowenthal MN, Horowitz J, Gaspar N, et al. Hyperreactive malarial splenomegaly and AIDS: proguanil prevents recurrent pneumonia. Trans R Soc Trop Med Hyg. 1996;90:313-4.
¹²
Hoffman SL, Piessens WF, Ratiwayanto S, et al. Reduction of suppressor T lymphocytes in the tropical splenomegaly syndrome. N Engl J Med. 1984;310:337-41.

Publication Dates

Publication in this collection
Sept-Oct 2014

History

Received
21 Mar 2014
Accepted
21 Apr 2014

This is an Open Access article distributed under the terms of the Creative Commons Attribution-Noncommercial No Derivative License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium provided the original work is properly cited and the work is not changed in any way.

[1] ¹
Bryceson A, Fakunle YM, Fleming AF, et al. Malaria and splenomegaly (letter). Trans R Soc Trop Med Hyg. 1983;77: 879.

[2] ²
Crane GG. Recent studies of hyperreactive malarious splenomegaly (tropical splenomegaly syndrome) in Papua New Guinea. P N G Med J. 1986;29:35-40.

[3] ³
Doenças Infecciosas e Parasitárias: Enfoque Amazônico/Raimundo Nonato Queiroz de Leão {coordenador}. Belém: Cejup, UEPA, Instituto Evandro Chagas; 1997.

[4] ⁴
Fakunle YM. Tropical splenomegaly. Clin Hematol. 1981;10:963-75.

[5] ⁵
Bates I, Bedu-Addo G. Review of diagnostic criteria of hyperreactive malarial splenomegaly. Lancet. 1997;349: 1179.

[6] ⁶
Alecrim, WD. Estudo clínico e epidemiológico da malária no Rio Ituxi-Amazonas. 1979. 115p. Tese (mestrado). Universidade de Brasiília, Brasília. 1979.

[7] ⁷
Bhatia KK, Crane GG. HLA heterozygosity and hyperreactive malarious splenomegaly in the Upper Watut Valley of Nova Guinéa. P N G Med J. 1989;32:277-86.

[8] ⁸
Kelly KM. IGHG3 G and the pathogenesis of hyperreactive malarious splenomegaly. Med Hypotheses. 1996;46:135-9.

[9] ⁹
Ranjan K, Singh. Hyperreactive malarial splenomegaly in expatriates. Travel Med Infect Dis. 2007;5:24-9.

[10] ¹⁰
De Iaco G, Saleri N, Perandin F, et al. Case Report. Hyper-reactive malarial splenomegaly in a patient with human immunodeficiency virus. Am J Trop Med Hyg. 2008;78:239-40.

[11] ¹¹
Lowenthal MN, Horowitz J, Gaspar N, et al. Hyperreactive malarial splenomegaly and AIDS: proguanil prevents recurrent pneumonia. Trans R Soc Trop Med Hyg. 1996;90:313-4.

[12] ¹²
Hoffman SL, Piessens WF, Ratiwayanto S, et al. Reduction of suppressor T lymphocytes in the tropical splenomegaly syndrome. N Engl J Med. 1984;310:337-41.

	Admission	1 month	9 month
Hb (g/dL)	5.6	10.2	13.7
Platelets/mL	56,000	100,000	99,000
Leukocytes (μ/L)	4300	3500	5800
IgM (mg/dL)	1790	–	473
Protein electrophoresis (Hypergamma %)	51	35.8	30
Albumin (g/dL)	2.5	4.5	4.68
Spleen volume CT abdomen (vol/mL)	3700	–	1358

Major criteria	Minor criteria
Splenomegaly > 10 cm	Hepatic sinusoidal lymphocytosis
IgM > 2SD of local mean	Hypersplenism
High titers of antimalarial antibodies	Lymphocytic proliferation
Clinical and immunological response to antimalarial drug	Normal cellular and humoral immune response to antigenic challenge excluding Plasmodium Occurrence within families and Tribes

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