Your search keyword '"Ilyas Kamboh, M"' showing total 3 results

1. APOE genetic associations with seizure development after severe traumatic brain injury.

Author

Miller, Megan A., Conley, Yvette, Scanlon, Joelle M., Ren, Dianxu, Ilyas Kamboh, M., Niyonkuru, Christian, and Wagner, Amy K.

Subjects

ANTICONVULSANTS, BRAIN damage complications, AMYLOIDOSIS, ANALYSIS of variance, APOLIPOPROTEINS, BRAIN damage, CHI-squared test, COMA, SEIZURES (Medicine), DISEASE susceptibility, FISHER exact test, GENES, LENGTH of stay in hospitals, INTENSIVE care units, MORTALITY, NURSING assessment, HEALTH outcome assessment, POLYMERASE chain reaction, PROBABILITY theory, RESEARCH funding, SPASMS, T-test (Statistics), WHITE people, GENETIC testing, RETROSPECTIVE studies, SEVERITY of illness index, ANALYTICAL chemistry, GENETICS, PATHOLOGY, PHYSIOLOGY, PATHOLOGICAL physiology

Abstract

Primary objective: The purpose of the current study is to assess the role of the APOE genotype in post-traumatic seizure (PTS) development. Research design: A retrospective study of 322 adult Caucasians with a severe TBI and APOE genotype. Methods and procedures: Medical records were searched for PTS. Time to first seizure was categorized as early, late or delayed-onset PTS. Potential PTS associations by genotype, grouped genotype and allele were investigated. Main outcome and results: No statistically significant associations were found. However, two out of the four individuals (50%) with the E4/E4 genotype had late/delayed-onset PTS. Furthermore, none with a E2/E2 or E2/E4 genotype seized in the late periods. Conclusions: The results of this study may suggest 4/4 as a risk genotype for late/delayed onset PTS and a potential neuroprotective role of the E2 allele. However, this study did not definitively support a role for the APOE genotype in PTS susceptibility and indicates that larger populations are needed to fully evaluate the potential impact of APOE on PTS. [ABSTRACT FROM AUTHOR]

Published

2010

2. Genetic variation in apolipoprotein H (β2-glycoprotein I) affects the occurrence of antiphospholipid antibodies and apolipoprotein H concentrations in systemic lupus erythematosus.

Author

Ilyas Kamboh, M., Manzi, S., Mehdi, H., Fitzgerald, S., Sanghera, D.K., Kuller, L.H., and Atson, C.E.

Subjects

*APOLIPOPROTEINS, *PHOSPHOLIPID antibodies, *SYSTEMIC lupus erythematosus, *HUMAN genetic variation

Abstract

Apolipoprotein H (apoH, protein; APOH, gene) is a required cofactor for the production of antiphospholipid antibodies (APA). In this study we have examined whether genetic variation in the APOH gene affects variation in risk for systemic lupus erythematosus (SLE), occurrence of antiphospholipid antibodies (APA), anti-apoH, and plasma apoH concentrations. A total of 222 white SLE women were screened for four APOH polymorphisms (codons 88, 247, 306, and 316) by polymerase chain reaction, and for plasma apoH concentrations by ELISA. Of these, 29.3% were positive for APA (APA-positive group) and 31.1% for anti-apoH. None of the four APOH polymorphisms were significantly associated with variation in risk for SLE. The codons 306 and 316 polymorphisms showed significant, gene-dosage effects on plasma apoH concentrations (P<0.0001) and explained 30% and 13%, respectively, of the residual variation in apoH concentrations. No significant association was observed between anti-apoH status and APOH polymorphisms or plasma apoH levels. However, plasma apoH concentrations were significantly higher in patients positive for APA than in patients negative for APA (18.5±4.0 mg/dl vs 17.1±3.8 mg/dl; P=0.02). The distribution of the Trp316Ser polymorphism was significantly different between the APA-positive and APA-negative groups. The frequency of the mutant allele (Ser316) was significantly lower in the APA-positive group than the APA-negative group (3.1% vs 12.1% P<0.04), indicating that the Ser316 mutation is protective against the production of phospholipid-apoH dependent APA. Our data indicate that common genetic variation in the APOH gene is a significant determinant of plasma apoH variation in SLE patients, and the Trp316Ser polymorphism appears to provide protection against the production of APA in SLE patients. [ABSTRACT FROM AUTHOR]

Published

1999

3. Distribution of plasma α1-antichymotrypsin levels in Alzheimer disease patients and controls and their genetic controls

Author

Wang, Xiaoyan, DeKosky, Steven T., Ikonomovic, Milos D., and Ilyas Kamboh, M.

Subjects

*ALZHEIMER'S disease, *BLOOD plasma

Abstract

Alzheimer’s disease (AD) is a complex multifactorial disease in which many genetic and environmental factors are involved. Recent studies have shown that α1-antichymotrypsin (ACT) is one of the candidate genes for AD. Elevated levels of ACT have been widely, but not universally reported in the cerebrospinal fluid and plasma of AD patients. The genetic association between the ACT/codon -17*A allele of the signal peptide polymorphism and AD has been shown in some studies. One hypothesis is that the ACT/codon -17*A allele is in linkage disequilibrium with unknown functional mutation(s) in the ACT gene. Alternatively, the more hydrophobic character of the alanine (codon -17*A) may enhance ACT translocation into the endoplasmic reticulum and the Golgi apparatus, thus being secreted at higher levels. Therefore, this study was undertaken to determine the distribution of ACT plasma levels in cases (n = 397) and controls (n = 118) and the impact of ACT polymorphisms, including codon –17, on plasma ACT levels. In our cohort, plasma ACT levels were significantly higher in AD patients than controls (542.13 ± 7.11 mg/liter vs. 496.62 ± 12.79 mg/liter; P = 0.002). The ACT/codon –17 polymorphism showed significant association with ACT levels in male AD patients, while the effect of the intron 4 polymorphism was significant in both male and female patients. Codon 227 polymorphism was associated with lower ACT levels in AD patients. In conclusion, ACT may play an important role in the AD pathogenesis and genetic variation in the ACT gene appears to have some effect on plasma ACT concentrations. [Copyright &y& Elsevier]

Published

2002