30 research outputs found
Isolation of Mycobacterium monacense from chemoport: A rare case report and review of literature
We report a rare case of Mycobacterium monacense isolated from the blood of a patient with carcinoma breast with an infected chemoport. Initial blood cultures from peripheral line and port were sterile. Repeated blood cultures signaled positive which showed weakly stained gram positive bacilli on smear from both the vials. Nontuberculous Mycobacterial infection and speciation were confirmed by real time polymerase chain reaction and sequencing. Chemoport was removed and patient responded to 3 drug regimen with Rifampicin, Ethambutol and Clarithromycin therapy with no recurrence at 15 month follow-up
Reversible paraneoplastic encephalomyelitis as the presenting feature of ovarian teratoma: A clinicopathological correlate
Paraneoplastic encephalomyelitis (PEM) is a well-characterized neurological syndrome. Its association with ovarian teratoma is rare. A young lady presented with features suggestive of encephalomyelitis with predominant cerebellar syndrome. Magnetic resonance imaging brain was normal. Cerebrospinal fluid showed lymphocytic pleocytosis. Computerized tomography scan of the pelvis revealed a complex left ovarian cyst. With a clinical diagnosis of PEM she underwent a left salpingo-oopherectomy. This was followed by total recovery of the PEM in two weeks. The histopathology revealed immature teratoma. The interesting feature was the clinicopathological correlation between the finding of fetal cerebellar tissue in the tumor and the PEM with predominant cerebellar features
Association of CYP3A5*3 polymorphism with development of acute leukemia
Background : CYP3A5 was observed to be an important genetic contributor
to inter individual differences in CYP3A-dependent drug metabolism in
acute leukemic patients. Loss of CYP3A5 expression was mainly conferred
by a single nucleotide polymorphism at 6986A>G (CYP3A5*3). We
investigated the association between CYP3A5*3 polymorphism and acute
leukemia. Materials and Methods : Two hundred and eighty nine acute
leukemia cases comprising of 145 acute lymphocytic leukemia (ALL), 144
acute myeloid leukemia and 241 control samples were analyzed for
CYP3A5*3 polymorphism using PCR-RFLP method. Statistical analysis was
performed with SPSS version (15.0) to detect the association between
CYP3A5*3 polymorphism and acute leukemia. Results : The CYP3A5*3
polymorphism 3/3 genotype was significantly associated with acute
leukemia development (\u3c72 - 133.53; df-2, P 0.000). When the data
was analyzed with respect to clinical variables, mean WBC, blast % and
LDH levels were increased in both ALL and AML cases with 3/3 genotype.
The epidemiological variables did not contribute to the genotype risk
to develop either AML or ALL. Conclusion : The results suggest that the
CYP3A5*3 polymorphism might confer the risk to develop ALL or AML
emphasizing the significance of effective phase I detoxification in
carcinogenesis. Association of the polymorphism with clinical variables
indicate that the 3/3 genotype might also contribute to poorer survival
of the patients
Association of CYP3A5*3 polymorphism with development of acute leukemia
Background : CYP3A5 was observed to be an important genetic contributor to inter individual differences in CYP3A-dependent drug metabolism in acute leukemic patients. Loss of CYP3A5 expression was mainly conferred by a single nucleotide polymorphism at 6986A>G (CYP3A5FNx013). We investigated the association between CYP3A5FNx013 polymorphism and acute leukemia.
Materials and Methods : Two hundred and eighty nine acute leukemia cases comprising of 145 acute lymphocytic leukemia (ALL), 144 acute myeloid leukemia and 241 control samples were analyzed for CYP3A5FNx013 polymorphism using PCR-RFLP method. Statistical analysis was performed with SPSS version (15.0) to detect the association between CYP3A5FNx013 polymorphism and acute leukemia.
Results : The CYP3A5FNx013 polymorphism 3/3 genotype was significantly associated with acute leukemia development (χ2 - 133.53; df-2, P 0.000). When the data was analyzed with respect to clinical variables, mean WBC, blast % and LDH levels were increased in both ALL and AML cases with 3/3 genotype. The epidemiological variables did not contribute to the genotype risk to develop either AML or ALL.
Conclusion : The results suggest that the CYP3A5FNx013 polymorphism might confer the risk to develop ALL or AML emphasizing the significance of effective phase I detoxification in carcinogenesis. Association of the polymorphism with clinical variables indicate that the 3/3 genotype might also contribute to poorer survival of the patients