Familial Hemophagocytic Lymphohistiocytosis secondary to UNC13D mutation: a report of two cases

The first case was a 15-month-old male infant born to consanguineous parents via normal vaginal delivery. He had normal growth and development until admission due to prolonged fever for 40 days with no specific pattern, vomiting, and maculopapular rash on his face. His physical examination revealed huge splenomegaly (diameter 120 mm) and fever. Liver function tests demonstrated a rise in aspartate aminotransferase (AST) of 88 IU/L and alanine aminotransferase (ALT) of 52 IU/L. His Complete blood count (CBC) showed bicytopenia (white blood cell count of 10.8 thousand/mm³, anemia with hemoglobin of 10.8 g/dl, and thrombocytopenia with a platelet count of 106 *103/μl). Triglyceride (TG) level was initially 425 mg/dl, which increased to 644 mg/dl. The cholesterol level was initially 86 mg/dl, which increased to 182 mg/dl. The c-reactive protein (CRP) was high (73 mg/dl) with a normal erythrocyte sedimentation rate (ESR) at the same time (14 mm/h). Remarkably, the value of serum ferritin was normal throughout all his disease period (150 μg/l).

His abdominal sonography illustrated splenomegaly with a diameter of 120 mm and homogenous echogenicity. Bone marrow aspiration (BMA) performed from the iliac crest appeared normal. He was diagnosed with macrophage activating syndrome in the context of systemic juvenile idiopathic arthritis by a consultant rheumatologist. He received intravenous methylprednisolone pulse therapy (30 mg/kg) and intravenous immune globulin (IVIG). He was discharged from the hospital with oral prednisolone at a dose of 1 mg/kg/day and readmitted with intermittent fever and vomiting after 45 days. He had bicytopenia, increased ALT and CRP during hospitalization, and his ferritin level was 248 μg/l. Antibody assessment against cytomegalovirus (CMV) and Epstein-Barr virus (EBV) displayed no abnormality.

The patient underwent BMA again, and bone marrow revealed abundant hemophagocytic cells. He was treated with cyclosporine A, etoposide, and dexamethasone according to HLH protocol 2004. After 1 month of treatment, CBC turned normal; CRP and TG decreased. Upon the completion of induction therapy with HLH protocol and initiation of maintenance therapy, the patient experienced a disease flare-up and was readmitted with fever and status epilepticus. Laboratory data revealed pancytopenia and increased levels of TG, AST, and ALT again; however, ferritin level was in the normal range, and brain computed tomography (CT) scan showed ventriculomegaly and Mega Cisterna Magna (Table 1).

In the last course of hospitalization, the patient passed away because of progressive brain involvement and hydrocephalus, and the whole-exome sequencing (on genomic DNA extracted from peripheral blood cells through an Agilent SureSelect V7 kit and Genome Analyzer HiSeq 4000 (Illumina, USA)) revealed a homozygous intronic UNC13D (NM_199242: c.2448-13G > A), probably affecting splicing. Although Sanger sequencing is not a routine survey for parents, since this mutation is transferred from parents or is a de novo mutation for the assessment of the next child, it was performed and confirmed that his parents were heterozygous carriers for this mutation (Fig. 1). The associated disease was Familial Hemophagocytic Lymphohistiocytosis 3(OMIM 608897) with autosomal recessive inheritance.

A 37-day-old female neonate born to consanguineous parents via cesarean section was admitted with fever (Temperature: 39 °C), cough, and a history of neonatal cholestasis. Her physical examination revealed fever and huge hepatosplenomegaly (with spleen preference). She had normal growth before admission despite the previous admission for cholestasis. Her liver function tests resulted in an AST of 33 IU/L that increased to 98 IU/L and an ALT of 21 IU/L that increased to 391 IU/L in her admission process. Her CBC revealed pancytopenia (leukopenia with white blood cell (WBC) of 3.13 thousand/mm³ and ANC of 210, anemia with hemoglobin of 5.1 g/dl, and thrombocytopenia with platelets of 41 *103/μl).

The TG and cholesterol levels were 113 mg/dl and 76 mg/dl, retrospectively. Ferritin level was increased to 2050 μg/l during her hospitalization. The CRP was 28 mg/L, and ESR was in the normal range (16 mm/h). Her abdominal sonography exhibited splenomegaly with a diameter of 144 mm and hepatomegaly with a diameter of 105 mm (both of homogenous echogenicity). The BMA and bone marrow biopsy were performed from the proximal tibia and appeared normal.

Her purified protein derivative (PPD) test turned negative, and a normal TORCH study (assessing antibodies against toxoplasmosis, rubella, CMV, and Herpes simplex virus [HSV]) was detected. The HIV ab was also negative. Metabolic screening tests, including MS/MS, ammonia, lactate, serum amino acid chromatography by HPLC, and urine reducing substance, all were normal. Nevertheless, the evaluation of Galactosemia, Gaucher’s disease, and Niemann-Pick’s disease were not feasible due to the previous history of blood transfusion. Furthermore, fibrinogen was in the normal range.

She was treated with prednisolone (4 mg/kg/day) and IVIG (2 g/kg Stat) as prescribed by a hematologist (with autoimmune thrombocytopenia and anemia diagnosis). Firstly, there was a rapid increase in platelet number and hemoglobin level. Nonetheless, the patient needed multiple blood transfusions and platelets due to sustained bicytopenia. Since the second case did not fulfill the criteria, she did not receive the 2004-HLH treatment protocol as suggested by a consultant rheumatologist. Finally, she died of severe sepsis by abdominal distention and positive blood culture with Pseudomonas aeruginosa. The whole-exome sequencing analysis detected a homozygous c.2448-13G > A UNC13D mutation, the same mutation observed in case 1. Sanger sequencing confirmed that his parents were also the heterozygous carriers of this mutation (data not shown). Sanger sequencing was performed since parents were young and desired to have a healthy child in the future.