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Loma Linda University

EducationLoma Linda, California, United States
About: Loma Linda University is a education organization based out in Loma Linda, California, United States. It is known for research contribution in the topics: Population & Medicine. The organization has 9220 authors who have published 13485 publications receiving 447094 citations. The organization is also known as: University of Loma Linda.


Papers
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Journal ArticleDOI
TL;DR: The interrater reliability of the Glasgow Coma Scale (GCS) between emergency physicians when adult patients with altered levels of consciousness are assessed was determined.

254 citations

Journal ArticleDOI
TL;DR: It was found that intrusion with the utility arch type of technique is not related to amount ofRoot shortening and the degree of root shortening was markedly higher in the maxilla than the mandible.

252 citations

Journal ArticleDOI
TL;DR: Policies in favor of the global adoption of plant-based diets will simultaneously optimize the food supply, health, environmental, and social justice outcomes for the world's population.

252 citations

Journal ArticleDOI
01 May 1998-Stroke
TL;DR: Greater NOS activity in core regions could explain in part the increased vulnerability of that region to ischemia and could theoretically contribute to the progression of the infarct over time.
Abstract: Background and Purpose—The present studies examined the hypothesis that the distribution of cerebral injury after a focal ischemic insult is associated with the regional distribution of nitric oxide synthase (NOS) activity. Methods—Based on previous studies that certain anatomically well-defined areas are prone to become either core or penumbra after middle cerebral artery occlusion (MCAO), we measured NOS activity in these areas from the right and left hemispheres in a spontaneously hypertensive rat filament model. Four groups were studied: (1) controls (immediate decapitation); (2) 1.5 hours of MCAO with no reperfusion (R0); (3) 1.5 hours of MCAO with 0.5 hour of reperfusion (R0.5); and (4) 1.5 hours of MCAO with 24 hours of reperfusion (R24). Three groups of corresponding isoflurane sham controls were also included: 1.5 (S1.5) or 2 (S2.0) hours of anesthesia and 1.5 hours of anesthesia+24 hours of observation (S24). Results—Control core NOS activity for combined right and left hemispheres was 129% grea...

251 citations

Journal ArticleDOI
TL;DR: The BMD phenotype can be partitioned into its genetic components and the effects of these loci on normal bone biology can be determined, and the BMD QTLs that are identified are in regions of the mouse genome that have known human homology, and will become useful experimental tools for mechanistic and therapeutic analyses of bone regulatory genes.
Abstract: Significant differences in vertebral (9%) and femoral (50%) adult bone mineral density (BMD) between the C57BL/6J (B6) and C3H/HeJ (C3H) inbred strains of mice have been subjected to genetic analyses for quantitative trait loci (QTL). Nine hundred eighty-six B6C3F2 females were analyzed to gain insight into the number of genes that regulate peak BMD and their locations. Femurs and lumbar vertebrae were isolated from 4-month-old B6C3F2 females at skeletal maturity and then BMD was determined by peripheral quantitative computed tomography (pQCT). Estimates of BMD heritability were 83% for femurs and 72% for vertebrae. Genomic DNA from F2 progeny was screened for 107 polymerase chain reaction (PCR)-based markers discriminating B6 and C3H alleles on all 19 autosomes. The regression analyses of markers on BMD revealed ten chromosomes (1, 2, 4, 6, 11, 12, 13, 14, 16, and 18) carrying QTLs for femurs and seven chromosomes (1, 4, 7, 9, 11, 14, and 18) carrying QTLs for vertebrae, each with log10 of the odds ratio (LOD) scores of 2.8 or better. The QTLs on chromosomes (Chrs) 2, 6, 12, 13, and 16 were unique to femurs, whereas the QTLs on Chrs 7 and 9 were unique to vertebrae. When the two bone sites had a QTL on the same chromosome, the same marker had the highest, although different, LOD score. A pairwise comparison by analysis of variance (ANOVA) did not reveal significant gene × gene interactions between QTLs for either bone site. BMD variance accounted for by individual QTLs ranged from 1% to 10%. Collectively, the BMD QTLs for femurs accounted for 35.1% and for vertebrae accounted for 23.7% of the F2 population variances in these bones. When mice were homozygous c3/c3 in the QTL region, 8 of the 10 QTLs increased, while the remaining two QTLs on Chrs 6 and 12 decreased, femoral BMD. Similarly, when mice were homozygous c3/c3 in the QTL region for the vertebrae, five of the seven QTLs increased, while two QTLs on Chrs 7 and 9 decreased, BMD. These findings show the genetic complexity of BMD with multiple genes participating in its regulation. Although 5 of the 12 QTLs are considered to be skeleton-wide loci and commonly affect both femurs and vertebrae, each of the bone sites also exhibited unique QTLs. Thus, the BMD phenotype can be partitioned into its genetic components and the effects of these loci on normal bone biology can be determined. Importantly, the BMD QTLs that we have identified are in regions of the mouse genome that have known human homology, and the QTLs will become useful experimental tools for mechanistic and therapeutic analyses of bone regulatory genes.

251 citations


Authors

Showing all 9287 results

NameH-indexPapersCitations
Bruce L. Miller1631153115975
Jonathan I. Epstein138112180975
Tony L. Yaksh12380660898
David M. Livingston11831258142
William B. Isaacs11752158187
Alan W. Partin11171054213
David N. Herndon108122754888
Edward R. Laws10572239822
David C. Bellinger9845235449
Pedram Argani9737235607
Michael W. Steffes9634143260
Gary K. Steinberg9452931259
Michael S. Gazzaniga9237235305
David J. Baylink9042529109
Jesse B. Jupiter9054326480
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Performance
Metrics
No. of papers from the Institution in previous years
YearPapers
202332
202267
2021904
2020823
2019727
2018638