A 16.5-year-old female was diagnosed to have GD following presentation with fatigability, weight loss, nervousness, tremors, delayed puberty, diffuse goiter and exophthalmos. The hyperthyroid status was confirmed biochemically as Thyroid Stimulating Hormone (TSH) was suppressed, free thyroxine (FT4) and free tri-iodothyronine (FT3) were elevated. Antibody testing for thyroid receptor and anti-thyroid peroxidase were not done due to the resources constraints. The presence of exophthalmos supported the clinical diagnosis of GD. Baseline Complete Blood Count (CBC) and liver function tests were normal (Table 1). She was commenced on carbimazole 10 mg BID and propranolol 10 mg TDS. The patient and her family were counseled about the therapy side effects and clear instructions were provided. She was then referred to be under the care of the nearby pediatrician.
She continued to follow up for the initial few months, then she dropped to do so though was adherent to her medication. Fourteen months later, she presented to the local hospital with shortness of breath and right hypochondrial pain. She was found to be very pale with anemic heart failure which necessitated an urgent blood transfusion and was then referred to the regional Pediatric Hospital. The patient and her family denied any history of bleeding, fever, bone pain or jaundice at that time. Further workup there revealed that she was hypothyroid (Table 1). Therefore, levothyroxine was started after carbimazole withdrawal. Unfortunately, CBC and blood biochemistry results were lost but no bone marrow examination was done. After five days, she was discharged home in a better condition and referred back to the local hospital for further follow-up. Unfortunately, she was not consistent to follow up and was not adherent to her medication (levothyroxine).
Eight months later, she was admitted again to the local hospital with a history of high grade fever, fatigue and bone pain for two weeks and was found to have severe anemia. She received blood transfusion, intravenous wide-spectrum antibiotics and was referred to our facility for further management. On arrival, she was cachexic, thyrotoxic with tachycardia, large collapsing pulse, wet warm hands, tremors, diffuse goiter and exophthalmos. In addition, she had cervical lymphadenopathy, parotid enlargement, fever, tender hepatomegaly, no splenomegaly and generalized bone tenderness. She was wasted (Body Mass Index -5.5 SDS), short (-3.8 SDS) and pre-pubertal. Laboratory investigations showed pancytopenia, atypical lymphocytes on peripheral film, thyrotoxicosis, elevated C-reactive protein and negative Ebstein Barr virus serology (Table 1). Renal and liver function tests as well as urinalysis and serum uric acid were normal. She was started on propranolol, intravenous wide-spectrum antibiotics, intravenous fluid and antipyretics for which she showed some improvement.
After consultation with a hematologist, a bone marrow examination was performed. It showed a hypercellular marrow, reduced megakaryocytes, depressed erythroid series and 80% infiltration with blast cells which were consistent with ALL. The patient was then transferred to the oncology unit for further management. Unfortunately, she passed away after initiation of chemotherapy with complications of tumor lysis syndrome.