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Journal of Postgraduate Medicine, Vol. 56, No. 4, October-December, 2010, pp. 301-302 Images in Pathology Hemophagocytosis in scrub typhus R Valsalan1, K Kosaraju2, T Sohanlal3, PS Prem Kumar4 1 Division of Medicine, Lyell McEwin Hospital, South Australia, Australia Correspondence Address: R Valsalan, Division of Medicine, Lyell McEwin Hospital, South Australia, Australia, drrohithv@gmail.com Date of Submission: 03-Feb-2010 Code Number: jp10088 PMID: 20935405 DOI: 10.4103/0022-3859.70949 Hemophagocytosis syndrome or hemophagocytic lymphohistiocytosis (HLH) is a rare hematological disorder characterized by febrile illness, cytopenia, lymphadenopathy and hepatosplenomegaly and hyperferritinemia. [1] Phagocytosis of blood cells and their precursors is a hallmark of hemophagocytic syndromes (HPS). Hemophagocytosis is achieved mostly by monocytes and macrophages, and nitro-blue tetrazolium reduction by monocytes from patients with HLH is approximately six times that of control monocytes. Excessive activation of monocytes in HLH may be due to stimulation by high levels of activating cytokines. High levels of interferon-γ (IFN-γ), soluble interleukin-2 receptor, tumor necrosis factor-α (TNF-α), interleukin-1, and interleukin-6 have been demonstrated, suggesting the elaboration of activating cytokines by T-helper cells or it can also result from poorly regulated or inappropriate Th1 responses to intracellular pathogens. The details of immunological protective mechanisms against rickettsial infections, including activation of cytokines, are not fully understood, but macrophages and T-cells are believed to play an important role in protection against rickettsial infections and appearance of HPS. HPS is caused by a number of viruses, including Cytomegalovirus (CMV), Epstein-Barr virus (EBV) and human herpes virus-6 as well as collagen-vascular diseases and malignancies, particularly T-cell lymphomas [2] . Hemophagocytosis causing pancytopenia is a medical emergency and is fatal despite aggressive treatment. We report a 22-year-old barber who came with acute febrile illness of 10 days duration. On examination he was pale and febrile (104Ί F). Non-tender small discrete lymph nodes were seen in the cervical region. Hepatosplenomegaly was present on abdominal examination. Cardiovascular, respiratory and central nervous system examinations were unremarkable. Complete blood picture revealed hemoglobin- 8.5 gm%, reticulocyte count 0.16%, WBC count 700 cells/mm 3 , shift to left with neutrophils 34%, lymphocytes 62%, monocytes 4%, platelet count 12,000 cells/mm 3 and ESRErythrocyte sedimentation rate) 120 mm/h. Renal, liver functions, X-ray and computed tomography reports of thorax were within normal limits. Bactec blood cultures were sterile. Widal test, Standard agglutination test for Brucella, ANA global and profile, HIV (Human Immunodeficiency Virus) ELISA (Enzyme Linked Immunosorbent Assay), ELISA for Hepatitis B surface antigen and antibodies to Hepatitis-C virus were negative. Serum ferritin was >2000 microgram/L. Patient was empirically started on Piperacillin-Tazobactum and Teicoplanin for febrile neutropenia. Bone marrow aspiration showed hypercellular marrow with marked suppression of erythropoeisis and megakaryopoeisis with increased leucopoiesis, toxic vacoulation and hemophagocytosis [Figure - 1] and [Figure - 2]. The fever continued to spike despite therapy. Three days after the antibiotics, patient developed maculo--papular rash involving the extremities, palms and soles but sparing facial region [Figure - 3]. The antibiotics were stopped suspecting drug-induced rash. He was empirically started on Doxycycline 100 mg twice daily. Meanwhile, Weil-Felix test showed titers: OX-19: 40, OX-2: 160, OX-K: 320. After 48 h of starting Doxycycline, patient showed a striking response with fever touching the baseline. He became afebrile and the rash started disappearing. Ten days following anti-rickettsial therapy, a repeat Weil Felix test demonstrated increasing titers: OX-2 and OX-19- negative OX K 1: 320 and blood picture showed hemoglobin- 9.8 gm%, reticulocyte count 9%, WBC count 10,500 cells/mm 3 , platelet count1,74,000 cells/mm 3 and ESR 60 mm/h. IgM(Enzyme Linked Immunosorbent Serum Assay) ELISA for scrub typhus was positive with OD value (optical density) - 3.022 and cut-off OD - 0.225 (Scrub Typhus IgM ELISA-Inbios International). Scrub typhus is usually endemic in South East Asia, northern Australia and pacific islands. In India it has been reported from Himalayan regions, Haryana and southern India. [3] Scrub typhus presents as acute febrile illness which generally causes nonspecific symptoms and signs. The necrotic eschar is the pathognomonic feature, but is quite rare in the South East Asian population. [4] Thrombocytopenia has been reported in a few cases and is the result of consumption of platelets due to disseminated intravascular coagulation. [5] Our patient had all the features favoring HPS. The classical eschar noted in scrub typhus was not seen and could probably be due to the bite by the larval stage of mite. [6] Indirect immunofluorescence (IFA) is the gold standard test for scrub typhus, but ELISA is equally specific as IFA and more sensitive in the early phase of infection. [7] Our patient had high titers initially and the titers remained high even after one week which confirms scrub typhus infection. Mortality rates of untreated patients have ranged from 0-30%. [6] The prognosis of scrub typhus associated with HPS is unknown. In our patient, there was a clear association between scrub typhus and hemophagocytosis as was shown by the correct diagnosis of scrub typhus and the disappearance of the hemophagocytic phenomenon after successful treatment with specific chemotherapy. Pancytopenia associated with scrub typhus has been rarely reported in the medical literature;. [8] We believe it is important to consider scrub typhus as an important cause of bone marrow HPS in endemic areas like India. It is always beneficial to start anti-rickettsial chemotherapy empirically in these patients as the diagnostic facilities in most places are not readily available. References
Copyright 2010 - Journal of Postgraduate Medicine The following images related to this document are available:Photo images[jp10088f1.jpg] [jp10088f3.jpg] [jp10088f2.jpg] |
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