ABSTRACT
Background: co-inheritance of beta- and delta-globin mutations in Iran is not uncommon. This situation may interfere with correct diagnosis and genetic counseling of alpha- and beta-thalassemia in screening programs. Here we report the co-inheritance of beta- and delta-globin gene mutations in an individual with microcytosis, hypochromia and a normal hemoglobin A2 [HbA2] level
Methods: genomic DNA extraction, amplication refractory mutation system [ARMS] polymerase chain reaction and direct DNA sequencing of delta- and beta-globin genes were exploited for detection of the mutations in these two genes in an individual with low hematological indices and normal HbA2
Results: ARMS-PCR technique revealed the beta+ IVSI-5 [G to C] mutation and direct DNA sequencing of the delta-globin gene detected a previously reported delta codon 12 [AATàAAA] HbA2-NYU. This study reports HbA2-NYU in association with the beta IVSI-5 [G to C] mutation in Iran
Discussion: this report emphasizes that normal HbA2 expression in a beta-goblin carrier is due to mutation in the delta-globin gene and may cause misdiagnosis of thalassemia
ABSTRACT
Here we report the result of three cases referred to our lab that had a combination of beta-thalassemia and hemoglobin D [Hb D] traits. These individuals had no symptoms of profound anemia and hematological indices were similar to that of a beta-thalassemia heterozygote. In all three cases, the Hb D level was elevated and no HbA was detected electrophoretically. The electrophoresis pattern suggested that all cases were homozygotes for Hb D. PCR followed by digestion with EcoRI and sequencing of the beta-globin gene confirmed the presence of Cd 121 GAA>CAA in the heterozygous form with another beta-globin mutation. In all cases, the mutations in the beta-globin gene were detected by ARMS PCR technique and they were either IVSII-I or IVSI-5. Hematological studies of the family members showed that thalassemia which caused the mutations and Hb D were in the Trans position
ABSTRACT
Background: The antidiabetic and antilipaemic effects of Phoenix dactylifera leaf extract (PDE) and its fractions were investigated in various rat models. Methods: Diabetes was induced in male Wistar rats by alloxan monohydrate. Diabetic animals were randomly divided into 8 groups (1 diabetic control and 7 treated groups). Diabetic control animals received saline (5 mL/kg) orally, whereas the treatment groups received different doses of PDE (100, 200, and 400 mg/kg), PDE fractions (50, 100, and 200 mg/kg), or glibenclamide (4 mg/kg) orally once a day for 14 days. Blood was withdrawn for glucose determination on the 1st, 6th, 10th, and 14th days. The rats were fasted overnight and then sacrificed on the 14th day; blood was collected for biochemical evaluation, including the levels of blood glucose, plasma insulin, serum triglyceride, and cholesterol. Results: Subacute administration of PDE or its fractions in alloxan-induced diabetic rats significantly reduced blood glucose (P < 0.01). Water intake, serum triglyceride, and cholesterol also decreased in treated animals compared with the control group (P < 0.01). Plasma insulin level increased in the treated groups relative to the control group (P < 0.01). Conclusion: The results suggested that PDE exhibits antidiabetic and antilipaemic effects in alloxan-induced diabetic rats.