Your search keyword '"Gordon, R D"' showing total 9 results

1. Perturbed rotational structure in the 18 373 cm-1 band of the fluorescence excitation spectrum of jet-cooled chromyl fluoride.

Author

Gordon, R. D., Beattie, I. R., Brown, J. M., and Firth, S.

Subjects

*CHROMIUM compounds, *QUANTUM perturbations, *FLUORESCENCE, *ELECTRONIC excitation

Abstract

The 18 373 cm-1 band in the fluorescence excitation spectrum of jet-cooled CrO2F2 has been recorded with 0.007 cm-1 linewidth. The stronger lines have been assigned to a type c transition, consistent with a B1←A1 vibronic transition analogous to that in CrO2Cl2. Ground-state rotational constants, A″=0.148, B″=0.130, and C″=0.120 cm-1, agree well with electron diffraction predictions. The B1 excited state is significantly perturbed. Evidence includes (i) a decreasing fluorescence yield with increasing J′, such that signals were not observed for J′>3, (ii) the appearance of ‘‘extra’’ lines in the spectrum, leading to perturbing levels strongly mixed with levels of the B1 state, and (iii) anomalous effective rotational constants for the B1 state. [ABSTRACT FROM AUTHOR]

Published

1986

2. Salt, aldosterone and hypertension.

Author

Pimenta, E, Gordon, R D, and Stowasser, M

Subjects

*ALDOSTERONE, *HYPERTENSION, *SALT, *CARDIOVASCULAR diseases, *MORTALITY

Abstract

Clinical studies have shown that aldosterone and salt are independently related to hypertension, cardiovascular morbidity and mortality. More recently, studies in humans have demonstrated that, similarly to animals, endogenous aldosterone and dietary salt intake have not only separate, but also combined effects to accelerate target-organ deterioration. The aldosterone-salt interaction has important clinical implications, because combined effects of both can be minimized, if not avoided, by reducing salt intake. This interaction could also be interrupted by blocking the effects of aldosterone, with use of mineralocorticoid receptor antagonists, or by reducing aldosterone effects by adrenalectomy, in patients with aldosterone producing adenoma. Furthermore, aldosterone reduction or blockade may reduce salt appetite. [ABSTRACT FROM AUTHOR]

Published

2013

3. Unilateral adrenalectomy improves urinary protein excretion but does not abolish its relationship to sodium excretion in patients with aldosterone-producing adenoma.

Author

Pimenta, E, Gordon, R D, Ahmed, A H, Cowley, D, Robson, D, Kogovsek, C, and Stowasser, M

Subjects

*ADRENALECTOMY, *EXCRETION, *SODIUM, *ALDOSTERONE, *ADENOMA, *PROTEINURIA, *CARDIOVASCULAR diseases risk factors, *HYPERALDOSTERONISM

Abstract

Experimental and human data suggest that adverse cardiovascular (CV) and renal effects of aldosterone excess are dependent on concomitant dietary salt intake. Increased urinary protein (Uprot) is an early sign of nephropathy independently associated with CV risk. We have previously reported a positive association between Uprot and urinary sodium (UNa) in patients with hyperaldosteronism, but not in patients with normal aldosterone levels. We aimed to determine whether Uprot is related to UNa in patients with aldosterone-producing adenoma (APA) and whether the degree of Uprot and strength of this relationship is reduced following correction of hyperaldosteronism. Subjects with APA (n=24) underwent measurement of 24 h Uprot and UNa before and after unilateral adrenalectomy (follow-up 15.0±11.9 months). Following surgery, mean clinic systolic blood pressure fell (150.4±18.2 vs 134.5±14.5 mm Hg, P=0.0008), despite a reduction in number of antihypertensive medications, and Uprot (211.2±101.6 vs 106.0±41.8 mg per day, P<0.0001) decreased. There was a positive correlation between Uprot and UNa both before (r=0.5477, P=0.0056) and after (r=0.5097, P=0.0109) adrenalectomy. Changes in UNa independently predicted Uprot reduction (P=0.0189). These findings suggest that both aldosterone levels and dietary salt contribute to renal damage, and that once glomerular damage occurs it is not completely resolved following correction of hyperaldosteronism. Our study suggests that treatment strategies based on reduction of aldosterone effects, by adrenalectomy or mineralocorticoid receptor blockade, in conjunction with low-salt diet would provide additional target-organ protection in patients with primary aldosteronism. [ABSTRACT FROM AUTHOR]

Published

2011

4. Calcium antagonists and gastrointestinal haemorrhage: the balancing act.

Author

Gordon RD and Gordon, R D

Published

1996

5. Further study of chromosome 7p22 to identify the molecular basis of familial hyperaldosteronism type II.

Author

Carss, K. J., Stowasser, M., Gordon, R. D., and O'Shaughnessy, K. M.

Subjects

*HYPERALDOSTERONISM, *ALDOSTERONE, *GENETIC polymorphisms, *HYPERTENSION, *POLYMERASE chain reaction, *GENETIC mutation

Abstract

Familial hyperaldosteronism type II (FH-II) is an inherited form of hyperaldosteronism associated with hypertension in most patients. The mutations that cause FH-II are unknown, but linkage analysis has mapped them to chromosome 7p22. As FH-II is clinically indistinguishable from sporadic primary aldosteronism, a common and treatable condition, unravelling the cause of FH-II has important implications for these sporadic cases. To investigate whether FH-II is caused by large deletions or insertions, we examined the virtual karyotype of four pairs of affected and unaffected individuals using high-density bead chips. We also sequenced the coding regions of five 7p22 candidate genes that were prioritized because of their putative role in cell growth. We found no evidence of single-nucleotide polymorphism (SNP) copy number variation between pairs, and from the widest gap on the chip, chromosome 7p22 deletions or insertions exceeding ∼50 kb in these pedigrees can be excluded. We found 15 SNPs (two of which were novel), but none of them were non-synonymous and segregated with the disease in the FH-II pedigrees. We have been able to exclude large genomic deletions or insertions at 7p22 and refine the candidate gene list for this locus, but the mutations causing FH-II remain elusive. [ABSTRACT FROM AUTHOR]

Published

2011

6. Factors Affecting the Aldosterone/Renin Ratio.

Author

Stowasser, M., Ahmed, A. H., Pimenta, E., Taylor, P. J., and Gordon, R. D.

Subjects

*ALDOSTERONE regulation, *RENIN, *HYPERALDOSTERONISM, *SEROTONIN uptake inhibitors, *LIQUID chromatography-mass spectrometry, *ADRENERGIC beta blockers, *ACE inhibitors, *SPIRONOLACTONE

Abstract

Although the aldosterone/renin ratio (ARR) is the most reliable screening test for primary aldosteronism, false positives and negatives occur. Dietary salt restriction, concomitant malignant or renovascular hypertension, pregnancy and treatment with diuretics (including spironolactone), dihydropyridine calcium blockers, angiotensin converting enzyme inhibitors, and angiotensin receptor antagonists can produce false negatives by stimulating renin. We recently reported selective serotonin reuptake inhibitors lower the ratio. Because potassium regulates aldosterone, uncorrected hypokalemia can lead to false negatives. Beta-blockers, alphamethyldopa, clonidine, and nonsteroidal antiinflammatory drugs suppress renin, raising the ARR with potential for false positives. False positives may occur in patients with renal dysfunction or advancing age. We recently showed that (1) females have higher ratios than males, and (2) false positive ratios can occur during the luteal menstrual phase and while taking an oral ethynylestradiol/drospirenone (but not implanted subdermal etonogestrel) contraceptive, but only if calculated using direct renin concentration and not plasma renin activity. Where feasible, diuretics should be ceased at least 6 weeks and other interfering medications at least 2 before ARR measurement, substituting noninterfering agents (e. g., verapamil slowrelease ± hydralazine and prazosin or doxazosin) were required. Hypokalemia should be corrected and a liberal salt diet encouraged. Collecting blood midmorning from seated patients following 2-4 h upright posture improves sensitivity. The ARR is a screening test only and should be repeated once or more before deciding whether to proceed to confirmatory suppression testing. Liquid chromatography-tandem mass spectrometry aldosterone assays represent a major advance towards addressing inaccuracies inherent in other available methods. [ABSTRACT FROM AUTHOR]

Published

2012

7. Daclizumab is associated with decreased rejection and improved patient survival in renal transplant recipients.

Author

Morris, J. A., Hanson, J. E., Steffen, B. J., Chu, A. H., Chi-Burris, K. S., Gotz, V. P., and Gordon, R. D.

Subjects

*KIDNEY transplantation, *MONOCLONAL antibodies, *IMMUNOSUPPRESSIVE agents, *INTERLEUKIN-2, *TRANSPLANTATION of organs, tissues, etc., *PATIENTS

Abstract

Morris JA, Hanson JE, Steffen BJ, Chu AH, Chi-Burris KS, Gotz VP, Gordon RD. Daclizumab is associated with decreased rejection and improved patient survival in renal transplant recipients.Clin Transplant 2005 DOI: 10.1111/j.1399-0012.2005.00344.x.© Blackwell Munksgaard, 2005The present study investigated the safety of induction therapy with daclizumab (compared with no induction treatment), in adult renal transplant patients reported to the Scientific Registry of Transplant Recipients (SRTR) database between January 1, 1998 and July 27, 2003. Patients who were discharged from the hospital on mycophenolate mofetil, azathioprine, or sirolimus were divided into two groups: induction treatment with daclizumab (n = 8203) and no induction treatment (n = 25,368). Patient survival, death due to infection and death due to malignancy were evaluated at 1 and 3 yr post-transplantation. Rejection and graft survival were also examined. Kaplan–Meier and Cox regression models were used to evaluate outcomes. No significant differences were found between patients treated with daclizumab compared with patients who received no induction therapy for death due to infection or malignancy at 1 and 3 yr post-transplantation. Patients treated with daclizumab (compared with no induction treatment) had statistically significantly better survival rates at 1 (96.9% vs. 96.2%, p = 0.003) and 3 yr (92.4% vs. 91.4%, p = 0.004) although absolute differences were minimal. This was confirmed in the multivariable Cox regression analysis for patient death at 1 (HR = 0.77, p < 0.001) and 3 yr (HR = 0.83, p = 0.001) post-transplantation. Patients treated with daclizumab compared to no induction had lower rejection rates at 1 (13.1% vs. 17.3%, p < 0.001) and 3 yr post-transplantation (16.7% vs. 21.3%, p < 0.001). Cox regression confirmed a decreased risk for rejection at 1 (HR = 0.74, p < 0.001) and 3 yr (HR = 0.75, p < 0.001). Treatment with daclizumab was associated with reduced risk for graft loss at 1 (HR = 0.82, p < 0.001) and 3 years (HR = 0.86, p < 0.001). In conclusion, daclizumab was associated with a significantly reduced risk for rejection and graft loss compared with no induction treatment, and improved patient survival. In addition, daclizumab was not associated with an increase in risk of death due to infection or malignancy, when compared with no induction therapy. These findings demonstrate the short and long-term safety and efficacy of daclizumab in patients transplanted between January 1998 and July 2003. [ABSTRACT FROM AUTHOR]

Published

2005

8. Increased severity of multifocal renal arterial fibromuscular dysplasia in smokers.

Author

Bofinger, A M, Hawley, C M, Fisher, P M, Daunt, N, Stowasser, M, and Gordon, R D

Subjects

*DYSPLASIA, *RENOVASCULAR hypertension, HEALTH of cigarette smokers

Abstract

Renal arterial fibromuscular dysplasia (FMD) is a significant cause of renovascular hypertension, especially in younger females. Tobacco constituents have been shown to stimulate proliferation and synthetic activity of cultured human vascular smooth muscle cells. We examined the relationship between smoking and severity of FMD in a group of 50 subjects with the multifocal form of renal arterial FMD. A detailed smoking history was obtained by interview, clinical data at diagnosis of FMD were obtained from medical records, and angiograms were reviewed. Clinical and angiographic features were compared between smokers and non-smokers. Twenty-four subjects were smokers. At the time of diagnosis of FMD, smokers were of younger mean age than non-smokers (38.7 years vs 48.9 years, P < 0.01), had a shorter median history of hypertension (1.5 years vs 8.5 years, P < 0.05), and had a higher prevalence of unilateral renal atrophy (67% vs 27%, P < 0.01). The distribution of age at diagnosis of FMD was unimodal in non-smokers and bimodal, with a discrete group of younger subjects, in smokers. We conclude that cigarette smoking is associated with an earlier onset and increased severity of disease in a susceptible subgroup of patients predisposed to multifocal renal arterial FMD. [ABSTRACT FROM AUTHOR]

Published

1999

9. Linkage of Gordon’s syndrome to the long arm of chromosome 17 in a region recently linked to familial essential hypertension.

Author

O’Shaughnessy, K M, Fu, B, Johnson, A, and Gordon, R D

Subjects

*HYPERTENSION, *CHROMOSOMES, *FAMILIAL diseases

Abstract

Gordon's syndrome (GS) is a salt-sensitive, hyperkalaemic, familial hypertension syndrome which may masquerade in milder forms as essential hypertension. The response of hyperakalaemia to dietary salt restriction and to mineralocorticoids is heterogeneous, suggesting genetic heterogeneity. In a recently published study using small pedigrees, possible linkage of GS to chromosomes 1 and 17 was described. Studying the largest pedigree so far reported with GS, and using fluorescent-labelled microsatellite markers, we sought evidence of linkage to chromosomes 1 and 17. In this family there was no segregation of GS with any of the markers for chromosome 1. On chromosome 17, however, evidence of linkage was found with a maximum multipoint LOD score of 2.4 (the maximum LOD possible from the pedigree) over markers D17S250 and D17S934. This represents strong evidence in this pedigree for a responsible gene mutation on the long arm of chromosome 17. Recent reports of linkage for essential hypertension and, especially, familial essential hypertension within the same area of chromosome 17 containing the D17S934 marker raise the possibility that the same gene may be responsible for familial essential hypertension and for Gordon's syndrome. [ABSTRACT FROM AUTHOR]

Published

1998