Your search keyword '"Peter Castelluccio"' showing total 6 results

1. Elevated Cerebrospinal Fluid Tau Protein Concentrations on Admission Are Associated With Long-term Neurologic and Cognitive Impairment in Ugandan Children With Cerebral Malaria

Author

Chandy C. John, Robert O. Opoka, Richard Idro, Andrew J. Saykin, John M. Ssenkusu, Andrea L. Conroy, Peter Castelluccio, Dibyadyuti Datta, Gregory S. Park, and Paul Bangirana

Subjects

0301 basic medicine, Microbiology (medical), medicine.medical_specialty, 030231 tropical medicine, Tau protein, Malaria, Cerebral, Aftercare, tau Proteins, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Cerebrospinal fluid, Internal medicine, medicine, Humans, Cognitive Dysfunction, Uganda, Child, Articles and Commentaries, Coma, biology, business.industry, Acute kidney injury, medicine.disease, Confidence interval, Patient Discharge, 030104 developmental biology, Infectious Diseases, Cerebral Malaria, biology.protein, medicine.symptom, business, Neurocognitive, Biomarkers, Retinopathy

Abstract

Background Elevated concentrations of cerebrospinal fluid (CSF) tau, a marker of axonal injury, have been associated with coma in severe malaria (cerebral malaria [CM]). However, it is unknown whether axonal injury is related to long-term neurologic deficits and cognitive impairment in children with CM. Methods Admission CSF tau concentrations were measured in 145 Ugandan children with CM and compared to clinical and laboratory factors and acute and chronic neurologic and cognitive outcomes. Results Elevated CSF tau concentrations were associated with younger age, increased disease severity (lower glucose and hemoglobin concentrations, malaria retinopathy, acute kidney injury, and prolonged coma duration, all P < .05), and an increased CSF:plasma albumin ratio, a marker of blood–brain barrier breakdown (P < .001). Admission CSF tau concentrations were associated with the presence of neurologic deficits at hospital discharge, and at 6, 12, and 24 months postdischarge (all P ≤ .02). After adjustment for potential confounding factors, elevated log10-transformed CSF tau concentrations correlated with worse cognitive outcome z scores over 2-year follow-up for associative memory (β coefficient, –0.31 [95% confidence interval [CI], –.53 to –.10]) in children Conclusions Acute axonal injury in children with CM is associated with long-term neurologic deficits and cognitive impairment. CSF tau concentrations at the time of the CM episode may identify children at high risk of long-term neurocognitive impairment.

Published

2019

2. Influence ofADH1B polymorphism on alcohol use and its subjective effects in a Jewish population

Author

Lucinda G. Carr, Ting-Kai Li, Trent R. Stewart, Howard J. Edenberg, Tatiana Foroud, and Peter Castelluccio

Subjects

Adult, Male, Adolescent, Alcohol Drinking, Population, Ethnic group, Alcohol, Locus (genetics), Biology, chemistry.chemical_compound, Gene Frequency, Genotype, Humans, Allele, education, Allele frequency, Genetics (clinical), Genetics, education.field_of_study, Polymorphism, Genetic, Ethanol, Alcohol Dehydrogenase, ADH1B, Middle Aged, chemistry, Jews, Female, Demography

Abstract

Class I alcohol dehydrogenases (ADHs) are the principal enzymes responsible for ethanol metabolism in humans. Genetic polymorphism at the ADH1B locus (old nomenclature ADH2) results in isozymes with quite different catalytic properties. The frequency of the ADH1B*2 allele varies among ethnic groups. ADH1B*2 is most often observed in Asian populations, and has been shown to be protective against alcoholism. The Jewish population has a higher frequency of the ADH1B*2 allele and lower rates of alcohol-related problems as compared to other Caucasian populations. Thus, it would be of interest to determine whether the ADH1B*2 allele is associated with alcohol consumption and its subjective effects in this group. Four groups of Jewish subjects (male and female college-age samples, and male and female general samples) were recruited from the same region of the United States. All subjects completed a questionnaire to delineate alcohol consumption and its subjective consequences. Genotype at the ADH1B locus was determined for each participant. ADH1B*2 allele frequencies were similar for the Jewish college-age and general population samples. Men in both the college-age and general population in the ADH1B*2 group reported more unpleasant reactions following alcohol consumption than men in the ADH1B*1 group. Men in the general population in the ADH1B*2 group drank alcohol less frequently than men who were homozygous ADH1B*1; there was a similar trend among the women. The ADH1B polymorphism is associated with unpleasant reactions after alcohol consumption, and frequency of alcohol consumption in these Jewish samples. © 2002 Wiley-Liss, Inc.

Published

2002

3. [Untitled]

Author

Robert B. Stewart, Peter Castelluccio, Tatiana Foroud, Aimee Ritchotte, Paula J. Bice, Ting-Kai Li, Lucinda G. Carr, Ronghai Bo, and L. Lumeng

Subjects

Genetics, food and beverages, Chromosome, Alcohol, Biology, Quantitative trait locus, chemistry.chemical_compound, Chromosome 16, Chromosome 3, chemistry, Chromosome 18, Saccharin, psychological phenomena and processes, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, Synteny

Abstract

The inbred preferring (iP) and nonpreferring (iNP) rat strains were derived from the selectively bred alcohol-preferring (P) and alcohol-nonpreferring (NP) lines. Previously, 381 iP × iNP F2 progeny were generated to identify quantitative trait loci (QTLs) influencing alcohol consumption and preference. Saccharin consumption (ml/48 h) and saccharin intake (ml/kg/day) were also measured in the F2 sample and were significantly correlated with both alcohol consumption and preference (all r ≥ .20, p < .0001), suggesting that there might be some QTLs influencing both saccharin and alcohol phenotypes. We have performed a genome screen using F2 animals with extreme saccharin or alcohol consumption to identify QTLs contributing to saccharin-related phenotypes. Lod scores greater than 2.0 were found on chromosomes 3, 16 and 18 in this sample. Additional genotyping was performed in these regions in the full sample of 381 F2 progeny to further characterize these putative QTLs. On chromosome 3, the maximum lod score in the full sample was 2.7 with saccharin consumption. This QTL appears to overlap with a QTL identified for alcohol consumption in the iP and iNP lines and has pleiotropic effects on both phenotypes. Interestingly, this region of rat chromosome 3 is syntenic with mouse chromosome 2, where a QTL influencing alcohol preference has been previously reported. The QTL on chromosome 16 has a maximum lod score of 4.0 with saccharin intake and 2.6 with saccharin consumption. The QTL on chromosome 18 has a maximum lod score of 2.7 with saccharin consumption. Taken together, these data provide the first results of a genome screen for QTLs contributing to saccharin phenotypes in the rat.

Published

2002

4. Suggestive evidence of a locus on chromosome 10p using the NIMH genetics initiative bipolar affective disorder pedigrees

Author

Sylvia G. Simpson, John I. Nurnberger, Dean F. MacKinnon, Theodore Reich, Howard J. Edenberg, Francis J. McMahon, Alison Goate, Carrie Smiley, Peter Castelluccio, Marvin J. Miller, Laura J. Bierut, Sevilla D. Detera-Wadleigh, Daniel L. Koller, Mary C. Blehar, Juliet J. Guroff, Judith A. Badner, Lynn R. Goldin, John P. Rice, Elliot S. Gershon, Elizabeth S. Bowman, N. Leela Rau, Melvin G. McInnis, J. Raymond DePaulo, O. Colin Stine, Tatiana Foroud, and Christopher M. Armstrong

Subjects

Genetics, Psychosis, Genotype, medicine, Chromosome, Locus (genetics), Pedigree chart, Bipolar disorder, Biology, medicine.disease, Genetics (clinical), Genetic determinism, Lod score

Abstract

As part of a four-center NIMH Genetics Initiative on Bipolar Disorder, a genome screen using 365 markers was performed on 540 DNAs from 97 families, enriched for affected relative pairs. This is the largest uniformly ascertained and assessed linkage sample for this disease, and includes 232 subjects diagnosed with bipolar I (BPI), 32 with schizo-affective, bipolar type (SABP), 72 with bipolar II (BPII), and 88 with unipolar recurrent depression (UPR). A hierarchical set of definitions of affected status was examined. Under Model I, affected individuals were those with a diagnosis of BPI or SABP, Model II included as affected those fitting Model I plus BPII, and Model III included those fitting Model II plus UPR. This data set was previously analyzed using primarily affected sib pair methods. We report the results of nonparametric linkage analyses of the extended pedigree structure using the program Genehunter Plus. The strongest finding was a lod score of 2.5 obtained on chromosome 10 near the marker D10S1423 with diagnosis as defined under Model II. This region has been previously implicated in genome-wide studies of schizophrenia and bipolar disorder. Other chromosomal regions with lod scores over 1.50 for at least one Model Included chromosomes 8 (Model III), 16 (Model III), and 20 (Model I). Am. J. Med. Genet. (Neuropsychiatr. Genet.) 96:18-23, 2000

Published

2000

5. [Untitled]

Author

Aimee Ritchotte, Ronghai Bo, Tatiana Foroud, Paula J. Bice, Peter Castelluccio, Lawrence Lumeng, Laurie Miller, Lucinda G. Carr, and Ting-Kai Li

Subjects

Genetics, Candidate gene, Chromosome 16, Chromosome, Biology, Quantitative trait locus, Selective breeding, Inbreeding, Genotyping, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, Chromosome 12

Abstract

Selective breeding has been employed to develop high-alcohol-drinking (HAD) and low-alcohol-drinking (LAD) rat lines from the heterogeneous N/Nih rat. Within-family selection and a rotational breeding design were used to discourage inbreeding (Li et al, 1993). To identify quantitative trait loci (QTLs) contributing to alcohol consumption, reciprocal HAD and LAD matings in conjunction with F1 intercrosses were used to create 459 F2 progeny. Using selective genotyping of 151 F2 progeny with extreme alcohol consumption scores and a novel least squares method developed by Haley et al (1994), five chromosomal regions (1, 5, 10, 12, and 16) were identified with lod scores greater than 2.0. Genotyping of the entire sample of 459 F2 progeny produced maximum lod scores of 3.5 on chromosome 5, 2.4 on chromosome 10, 4.7 on chromosome 12 and 2.9 on chromosome 16. The evidence of linkage to chromosome 1 diminished substantially to a maximum lod score of 0.5 when all F2 progeny were genotyped. This study is the first genome-wide study for QTLs underlying alcohol consumption that has employed noninbred lines. Further localization of these QTLs will likely provide insight and candidate genes for the study of human alcoholism.

Published

2000

6. Genomic screen for QTLs underlying alcohol consumption in the P and NP rat lines

Author

Lucinda G. Carr, Ting-Kai Li, Ronghai Bo, Lawrence Lumeng, Paula J. Bice, Peter Castelluccio, and Tatiana Foroud

Subjects

Genetic Markers, Candidate gene, Alcohol Drinking, Genotype, In Vitro Techniques, Quantitative trait locus, Biology, Selective breeding, Chromosomes, Quantitative Trait, Heritable, Genetics, Animals, Neuropeptide Y, Genetic Testing, Protein Precursors, Synteny, Genome, Chromosome, DNA, Rats, Genetic marker, Female, Lod Score, Inbreeding

Abstract

Selective breeding for voluntary alcohol consumption was utilized to establish the alcohol-preferring (P) and alcohol-nonpreferring (NP) rat lines. Inbreeding was initiated after 30 generations of selection and, after 19 generations of inbreeding, 384 F2 intercross progeny were created to identify quantitative trait loci (QTLs) influencing alcohol consumption. We had reported previously a QTL on Chromosome (Chr) 4; additional markers genotyped on Chr 4 have increased the maximum lod score from 8.6 to 9.2. This QTL acts in an additive fashion and continues to account for approximately 11% of the phenotypic variability. The 95% confidence interval is 12.5 cM and includes the candidate gene, neuropeptide Y. Subsequent to the identification of the QTL on Chr 4, a genome scan was completed to identify additional QTLs influencing alcohol consumption. A lod score of 2.5 was obtained on Chr 3, syntenic to a region previously reported for alcohol preference in mice. Analysis of Chr 8 produced a lod score of 2.2 near the dopamine D2 and serotonin 1b receptors, which have been previously reported as candidate genes for alcohol preference. Evidence for linkage to alcohol consumption was not found on any other chromosome. It therefore appears likely that, in addition to the QTL on Chr 4, multiple loci of small to moderate effect, such as those on Chrs 3 and 8, underlie the difference in alcohol consumption in the P/NP lines.

Published

1998