Your search keyword '"Montgomery, HE"' showing total 329 results

301. Genetic variation and the response to exercise.

Author

Montgomery HE

Subjects

Bone Density genetics, Bone and Bones physiology, Cardiovascular Diseases etiology, Cardiovascular Diseases prevention & control, Fibrinogen genetics, Fibrinogen metabolism, Heart Ventricles growth & development, Humans, Muscle, Skeletal physiology, Phenotype, Physical Endurance genetics, Physical Fitness physiology, Exercise physiology, Genetic Variation

Published

2001

302. The ACE I/D polymorphism and human physical performance.

Author

Woods DR, Humphries SE, and Montgomery HE

Subjects

Humans, Isoenzymes genetics, Peptidyl-Dipeptidase A genetics, Physical Fitness physiology, Polymorphism, Genetic genetics

Abstract

The D allele of the angiotensin-converting enzyme (ACE) I/D polymorphism is associated with elevated levels of serum and tissue ACE, increased production of the vasopressor angiotensin II and a reduction in the half-life of the vasodilator bradykinin. Several cardiac and renal conditions appear to have a worse prognosis in subjects homozygous for the D allele, whereas the I allele has been associated with enhanced endurance performance in elite distance runners, rowers and mountaineers. The nature of the gene-environment interaction between ACE I/D polymorphisms and physical training, an overview of recent findings and a discussion of possible underlying mechanisms is the subject of this review.

Published

2000

303. Genetics of inflammation and risk of coronary artery disease: the central role of interleukin-6.

Author

Woods A, Brull DJ, Humphries SE, and Montgomery HE

Subjects

Blood Coagulation physiology, Coronary Disease blood, Coronary Disease prevention & control, Genetic Markers genetics, Genetic Therapy, Humans, Inflammation blood, Inflammation complications, Interleukin-6 blood, Prognosis, Risk Factors, Transcription, Genetic, Coronary Disease etiology, Inflammation genetics, Interleukin-6 genetics

Published

2000

304. Raised blood pressure, not renin-angiotensin systems, causes cardiac fibrosis in TGR m(Ren2)27 rats.

Author

Bishop JE, Kiernan LA, Montgomery HE, Gohlke P, and McEwan JR

Subjects

Amlodipine therapeutic use, Angiotensin-Converting Enzyme Inhibitors therapeutic use, Animals, Animals, Genetically Modified, Antihypertensive Agents therapeutic use, Collagen analysis, Fibrosis, Hypertension metabolism, Hypertension pathology, Hypertrophy, Left Ventricular etiology, Hypertrophy, Left Ventricular metabolism, Hypertrophy, Left Ventricular pathology, Male, Mice, Myocardium chemistry, Peptidyl-Dipeptidase A blood, Ramipril therapeutic use, Rats, Rats, Sprague-Dawley, Time Factors, Hypertension complications, Myocardium pathology, Renin-Angiotensin System

Abstract

Objectives: Elevated systemic arterial blood pressure is associated with left ventricular hypertrophy and fibrosis. It has been suggested that both circulating and local myocardial renin-angiotensin systems play a role in mediating these responses. Here we describe the natural history of ventricular hypertrophy and fibrosis in the transgenic (mRen2)27 rat--a monogenetic model--which has a high tissue expression of the murine renin transgene, and suffers severe hypertension. We further explored the relative contribution of both hypertensive burden and circulating and tissue renin-angiotensin systems to the fibrotic process., Methods: The transgenic rats were treated from 28 days old with (1) a hypotensive dose of the ACE inhibitor ramipril which inhibited both tissue and circulating ACE activity, (2) the calcium antagonist amlodipine, or (3) a non-hypotensive dose of ramipril which inhibited about 60% of tissue ACE activity with little effect on circulating ACE. Normotensive Sprague-Dawley rats were used as controls., Results: The transgenics developed left ventricular hypertrophy along with perivascular and interstitial fibrosis which became progressively worse up to 24 weeks of age. Both the high dose of ramipril and amlodipine prevented the hypertrophy and fibrosis, whereas tissue ACE inhibition without lowering blood pressure had no effect, and actually led to a worsening of the fibrosis by 24 weeks., Conclusions: These results suggest that the development of left ventricular hypertrophy and fibrosis in the transgenic (mRen2)27 rat are regulated by blood pressure and not activity of the renin-angiotensin systems and that progression of fibrosis at 24 weeks involves a mechanism unrelated to local renin-angiotensin activity.

Published

2000

305. Measurement of the W-->taunu production cross section in pp collisions at square root s=1.8 TeV.

Author

Abbott B, Abolins M, Abramov V, Acharya BS, Adams DL, Adams M, Ahn S, Akimov V, Alves GA, Amos N, Anderson EW, Baarmand MM, Babintsev VV, Babukhadia L, Baden A, Baldin B, Banerjee S, Bantly J, Barberis E, Baringer P, Bartlett JF, Bassler U, Belyaev A, Beri SB, Bernardi G, Bertram I, Bezzubov VA, Bhat PC, Bhatnagar V, Bhattacharjee M, Blazey G, Blessing S, Boehnlein A, Bojko NI, Borcherding F, Brandt A, Breedon R, Briskin G, Brock R, Brooijmans G, Bross A, Buchholz D, Buescher V, Burtovoi VS, Butler JM, Carvalho W, Casey D, Casilum Z, Castilla-Valdez H, Chakraborty D, Chan KM, Chekulaev SV, Chen W, Cho DK, Choi S, Chopra S, Choudhary BC, Christenson JH, Chung M, Claes D, Clark AR, Cobau WG, Cochran J, Coney L, Connolly B, Cooper WE, Coppage D, Cullen-Vidal D, Cummings MA, Cutts D, Dahl OI, Davis K, De K, Del Signore K, Demarteau M, Denisov D, Denisov SP, Diehl HT, Diesburg M, Di Loreto G, Draper P, Ducros Y, Dudko LV, Dugad SR, Dyshkant A, Edmunds D, Ellison J, Elvira VD, Engelmann R, Eno S, Eppley G, Ermolov P, Eroshin OV, Estrada J, Evans H, Evdokimov VN, Fahland T, Feher S, Fein D, Ferbel T, Fisk HE, Fisyak Y, Flattum E, Fleuret F, Fortner M, Frame KC, Fuess S, Gallas E, Galyaev AN, Gartung P, Gavrilov V, Genik RJ Jr, Genser K, Gerber CE, Gershtein Y, Gibbard B, Gilmartin R, Ginther G, Gobbi B, Gómez B, Gómez G, Goncharov PI, González Solís JL, Gordon H, Goss LT, Gounder K, Goussiou A, Graf N, Grannis PD, Green DR, Green JA, Greenlee H, Grinstein S, Grudberg P, Grünendahl S, Guglielmo G, Gupta A, Gurzhiev SN, Gutierrez G, Gutierrez P, Hadley NJ, Haggerty H, Hagopian S, Hagopian V, Hahn KS, Hall RE, Hanlet P, Hansen S, Hauptman JM, Hays C, Hebert C, Hedin D, Heinson AP, Heintz U, Heuring T, Hirosky R, Hobbs JD, Hoeneisen B, Hoftun JS, Hsieh F, Ito AS, Jerger SA, Jesik R, Joffe-Minor T, Johns K, Johnson M, Jonckheere A, Jones M, Jöstlein H, Jun SY, Kahn S, Kajfasz E, Karmanov D, Karmgard D, Kehoe R, Kim SK, Klima B, Klopfenstein C, Knuteson B, Ko W, Kohli JM, Koltick D, Kostritskiy AV, Kotcher J, Kotwal AV, Kozelov AV, Kozlovsky EA, Krane J, Krishnaswamy MR, Krzywdzinski S, Kubantsev M, Kuleshov S, Kulik Y, Kunori S, Landsberg G, Leflat A, Lehner F, Li H, Li J, Li QZ, Lima JG, Lincoln D, Linn SL, Linnemann J, Lipton R, Lu JG, Lucotte A, Leuking L, Lundstedt C, Maciel AK, Madaras RJ, Manankov V, Mani S, Mao HS, Markeloff R, Marshall T, Martin MI, Martin RD, Mauritz KM, May B, Mayorov AA, McCarthy R, McDonald J, McKibben T, McMahon T, Melanson HL, Merkin M, Merritt KW, Miao C, Miettinen H, Mincer A, Mishra CS, Mokhov N, Mondal NK, Montgomery HE, Mostafa M, da Motta H, Nagy E, Nang F, Narain M, Narasimham VS, Neal HA, Negret JP, Negroni S, Norman D, Oesch L, Oguri V, Olivier B, Oshima N, Owen D, Padley P, Para A, Parashar N, Partridge R, Parua N, Paterno M, Patwa A, Pawlik B, Perkins J, Peters M, Piegaia R, Piekarz H, Pischalnikov Y, Pope BG, Popkov E, Prosper HB, Protopopescu S, Qian J, Quintas PZ, Raja R, Rajagopalan S, Reay NW, Reucroft S, Rijssenbeek M, Rockwell T, Roco M, Rubinov P, Ruchti R, Rutherfoord J, Santoro A, Sawyer L, Schamberger RD, Schellman H, Schwartzman A, Sculli J, Sen N, Shabalina E, Shankar HC, Shivpuri RK, Shpakov D, Shupe M, Sidwell RA, Singh H, Singh JB, Sirotenko V, Slattery P, Smith E, Smith RP, Snihur R, Snow GR, Snow J, Snyder S, Solomon J, Song XF, Sorín V, Sosebee M, Sotnikova N, Souza M, Stanton NR, Steinbrück G, Stephens RW, Stevenson ML, Stichelbaut F, Stoker D, Stolin V, Stoyanova DA, Strauss M, Streets K, Strovink M, Stutte L, Sznajder A, Tarazi J, Tartaglia M, Thomas TL, Thompson J, Toback D, Trippe TG, Turcot AS, Tuts PM, van Gemmeren P, Vaniev V, Varelas N, Volkov AA, Vorobiev AP, Wahl HD, Warchol J, Watts G, Wayne M, Weerts H, White A, White JT, Wightman JA, Willis S, Wimpenny SJ, Wirjawan JV, Womersley J, Wood DR, Yamada R, Yamin P, Yasuda T, Yip K, Youssef S, Yu J, Yu Y, Zanabria M, Zheng H, Zhou Z, Zhu ZH, Zielinski M, Zieminska D, Zieminski A, Zutshi V, Zverev EG, and Zylberstejn A

Abstract

We report on a measurement of sigma(pp-->W+X)B(W-->taunu) in pp collisions at sqrt[s]=1.8 TeV at the Fermilab Tevatron. The measurement is based on an integrated luminosity (lum) of 18 pb-1 of data collected with the D0 detector during 1994-1995. We find that sigma(pp-->W+X)B(W-->taunu)=2.22+/-0.09 (stat)+/-0. 10 (syst)+/-0.10 (lum) nb. Lepton universality predicts that the ratio of the tau and electron electroweak charged current couplings to the W boson, gWtau/gWe, be unity. We find gWtau/gWe=0.980+/-0.031, in agreement with lepton universality.

Published

2000

306. The ACE gene and muscle performance.

Author

Williams AG, Rayson MP, Jubb M, World M, Woods DR, Hayward M, Martin J, Humphries SE, and Montgomery HE

Subjects

Adult, Alleles, Genotype, Humans, Male, Muscle, Skeletal physiology, Physical Fitness, Muscle, Skeletal enzymology, Peptidyl-Dipeptidase A genetics, Physical Exertion

Published

2000

307. Endurance and the ACE I/D polymorphism.

Author

Woods DR, Brull D, and Montgomery HE

Subjects

Gene Expression Regulation, Enzymologic physiology, Gene Frequency genetics, Genetics, Population, Humans, Alleles, Genotype, Peptidyl-Dipeptidase A genetics, Physical Endurance genetics, Polymorphism, Genetic genetics

Abstract

A variant of the angiotensin-converting enzyme (ACE) gene, which we all carry, is known as the insertion, or I allele, due to the presence of a 287 base pair DNA fragment. This variant, or polymorphism, is associated with reduced levels of serum and tissue ACE. This intriguing polymorphism has been associated with various physiological and pathological states from diabetic renal disease to coronary heart disease. There have been conflicting reports regarding its association with some aspects of enhanced endurance performance in elite athletes. This review aims to examine the evidence for and against an association of the I allele with endurance and highlight some of the possible mechanism that might be involved. It is concluded that an association seems likely and that it is probably due to a local muscle effect rather than a central cardiorespiratory mechanism.

Published

2000

308. Gene-environment interaction in the determination of levels of plasma fibrinogen.

Author

Humphries SE, Luong LA, Montgomery HE, Day IN, Mohamed-Ali V, and Yudkin JS

Subjects

C-Reactive Protein, Electrophoresis, Fibrinogen metabolism, Genotype, Humans, Interleukin-6 genetics, Myocardial Ischemia blood, Myocardial Ischemia etiology, Polymorphism, Genetic, Risk Factors, Smoking blood, Fibrinogen genetics, Myocardial Ischemia genetics

Published

1999

309. Exercise training enhances endothelial function in young men.

Author

Clarkson P, Montgomery HE, Mullen MJ, Donald AE, Powe AJ, Bull T, Jubb M, World M, and Deanfield JE

Subjects

Administration, Sublingual, Adolescent, Adult, Blood Flow Velocity, Brachial Artery diagnostic imaging, Brachial Artery drug effects, Cholesterol, HDL blood, Endothelium, Vascular diagnostic imaging, Endothelium, Vascular drug effects, Fibrinogen metabolism, Follow-Up Studies, Humans, Lipoprotein(a) blood, Male, Military Personnel, Muscle, Smooth, Vascular diagnostic imaging, Muscle, Smooth, Vascular drug effects, Muscle, Smooth, Vascular physiology, Nitroglycerin administration & dosage, Predictive Value of Tests, Reference Values, Retrospective Studies, Ultrasonography, Doppler, Pulsed, Vasodilator Agents administration & dosage, Video Recording, Brachial Artery physiology, Endothelium, Vascular physiology, Exercise physiology, Vasodilation physiology

Abstract

Objectives: The present study was designed to assess whether exercise training can enhance endothelium-dependent dilatation in healthy young men., Background: Exercise has been shown to reduce cardiovascular morbidity and mortality, but the mechanisms for this benefit are unclear. Endothelial dysfunction is an early event in atherogenesis, and animal studies have shown that exercise training can enhance endothelial function., Methods: We have examined the effect of a standardized, 10-week, aerobic and anaerobic exercise training program on arterial physiology in 25 healthy male military recruits, aged 17 to 24 (mean 20) years, of average fitness levels. Each subject was studied before starting, and after completing the exercise program. Baseline vascular reactivity was compared with that of 20 matched civilian controls. At each visit, the diameter of the right brachial artery was measured at rest, during reactive hyperemia (increased flow causing endothelium-dependent dilation) and after sublingual glyceryltrinitrate (GTN; an endothelium-independent dilator), using high-resolution external vascular ultrasound., Results: At baseline, flow-mediated dilatation (FMD) and GTN-mediated dilatation were similar in the exercise and control groups (FMD 2.2+/-2.4% and 2.4+/-2.8%, respectively, p = 0.33; GTN 13.4+/-6.2 vs. 16.7+/-5.9, respectively, p = 0.53). In the military recruits, FMD improved from 2.2+/-2.4% to 3.9+/-2.5% (p = 0.01), with no change in the GTN-mediated dilation (13.4+/-6.2% vs. 13.9+/-5.8%, p = 0.31) following the exercise program., Conclusion: Exercise training enhances endothelium-dependent dilation in young men of average fitness. This may contribute to the benefit of regular exercise in preventing cardiovascular disease.

Published

1999

310. Gene-environment interaction in the determination of levels of haemostatic variables involved in thrombosis and fibrinolysis.

Author

Humphries SE, Henry JA, and Montgomery HE

Subjects

Adult, Age Factors, Aged, Alleles, Genotype, Hemostasis genetics, Humans, Middle Aged, Polymorphism, Genetic, Sex Factors, Fibrinogen genetics, Fibrinolysis genetics, Thrombosis genetics

Abstract

Although a specific genotype may be associated in healthy subjects with modest differences in levels of a risk factor for thrombosis, this effect may be larger or smaller in subgroups of subjects. Documenting such gene-environment interactions is important if genotype information is ever to be used in a clinical or diagnostic setting, and understanding the molecular mechanisms of such interactions is vital to be able to use the information to develop novel therapeutic approaches for reducing the risk of myocardial infarction. This review focuses on gene-environment interactions detected to date for the G-455A beta fibrinogen gene promoter polymorphism. Carriers of the A allele, representing roughly 20% of the population, consistently have on average 7-10% higher fibrinogen levels than those with the genotype GG. Data will be presented to demonstrate interaction between gender, smoking habit, age, presence of ischaemic disease and level of physical exercise, in the determination of the magnitude of this A-raising effect and thus on an individual's plasma fibrinogen levels.

Published

1999

311. Beyond coagulation: fibrinogen as a cause of cardiovascular surgical disease.

Author

Sumeray MS, Montgomery HE, and Humphries SE

Subjects

Blood Coagulation Disorders complications, Blood Coagulation Disorders therapy, Cardiovascular Diseases etiology, Cardiovascular Diseases surgery, Fibrinogen genetics, Genotype, Humans, Risk Factors, Blood Coagulation Disorders physiopathology, Cardiovascular Diseases physiopathology, Fibrinogen physiology

Abstract

Fibrinogen is generally considered to be an important mediator of clot formation. However, its effects on clots and perhaps other more direct effects may also make it a powerful mediator in the genesis and progression of atheromatous disease. Indeed, raised fibrinogen levels may pose as great a cardiovascular risk as classical risk factors such as elevated blood pressure or cholesterol levels. The plasma fibrinogen level of any given individual, and its associated cardiovascular risk, is dependent upon an interaction between environmental and intrinsic (genetic) factors. Most environmental factors associated with elevated fibrinogen levels are also potent cardiovascular risk factors (e.g., cigarette smoking). Less is known of the role played by genetic factors. However, as research into the genotypic influences on both basal and "stimulated" fibrinogen production continues, high-risk groups may be identified that may benefit from therapeutic intervention aimed at lowering plasma fibrinogen.

Published

1998

312. Human gene for physical performance.

Author

Montgomery HE, Marshall R, Hemingway H, Myerson S, Clarkson P, Dollery C, Hayward M, Holliman DE, Jubb M, World M, Thomas EL, Brynes AE, Saeed N, Barnard M, Bell JD, Prasad K, Rayson M, Talmud PJ, and Humphries SE

Subjects

Adult, Alleles, Gene Frequency, Genotype, Humans, Male, Middle Aged, Military Personnel, Mountaineering, Muscle, Skeletal physiology, Peptidyl-Dipeptidase A physiology, Physical Endurance physiology, Peptidyl-Dipeptidase A genetics, Physical Endurance genetics, Physical Fitness physiology

Published

1998

313. Association of angiotensin-converting enzyme gene I/D polymorphism with change in left ventricular mass in response to physical training.

Author

Montgomery HE, Clarkson P, Dollery CM, Prasad K, Losi MA, Hemingway H, Statters D, Jubb M, Girvain M, Varnava A, World M, Deanfield J, Talmud P, McEwan JR, McKenna WJ, and Humphries S

Subjects

Adult, Cohort Studies, Electrocardiography, Genotype, Heart Ventricles, Humans, Hypertrophy, Left Ventricular diagnostic imaging, Hypertrophy, Left Ventricular etiology, Male, Military Medicine, Natriuretic Peptide, Brain, Nerve Tissue Proteins metabolism, Alleles, Echocardiography, Peptidyl-Dipeptidase A genetics, Physical Education and Training, Polymorphism, Genetic

Abstract

Background: The absence (deletion allele [D]) of a 287-base pair marker in the ACE gene is associated with higher ACE levels than its presence (insertion allele [I]). If renin-angiotensin systems regulate left ventricular (LV) growth, then individuals of DD genotype might show a greater hypertrophic response than those of II genotype. We tested this hypothesis by studying exercise-induced LV hypertrophy., Methods and Results: Echocardiographically determined LV dimensions and mass (n=140), electrocardiographically determined LV mass and frequency of LV hypertrophy (LVH) (n=121), and plasma brain natriuretic peptide (BNP) levels (n=49) were compared at the start and end of a 10-week physical training period in male Caucasian military recruits. Septal and posterior wall thicknesses increased with training, and LV mass increased by 18% (all P<.0001). Response magnitude was strongly associated with ACE genotype: mean LV mass altered by +2.0, +38.5, and +42.3 g in II, ID and DD, respectively (P<.0001). The prevalence of electrocardiographically defined LVH rose significantly only among those of DD genotype (from 6 of 24 before training to 11 of 24 after training, P<.01). Plasma brain natriuretic peptide levels rose by 56.0 and 11.5 pg/mL for DD and II, respectively (P<.001)., Conclusions: Exercise-induced LV growth in young males is strongly associated with the ACE I/D polymorphism.

Published

1997

314. Gene-environment interaction in the determination of levels of haemostatic variables involved in thrombosis and fibrinolysis.

Author

Humphries SE, Panahloo A, Montgomery HE, Green F, and Yudkin J

Subjects

Chromosome Mapping, Fibrinogen genetics, Humans, Environment, Fibrinolysis genetics, Genetic Variation, Hemostasis genetics, Myocardial Ischemia genetics, Thrombosis genetics

Abstract

Functional sequence changes in the promoter of a gene may have a direct effect on the rate of transcription and thus on cellular or plasma levels of the protein. For both the beta fibrinogen gene and the plasminogen activator inhibitor-1 (PAI-1) gene such functional variations have been described. For the fibrinogen gene a G/A sequence variation has been detected at position -455 of the promoter, with carriers of the A allele, representing roughly 20% of the population, consistently having 7-10% higher fibrinogen levels than those with the genotype G/G. For the PAI-1 gene we have detected a run of four or five Guanidine residues (4G/5G polymorphism), and in several published studies those homozygous for the 4G allele (25% of the population) having levels of PAI-1 roughly 30% higher levels than 5G5G individuals. The magnitude of both of these genotype effects indicates that they are likely to be of biological significance in causing an elevated risk of thrombosis and reduced fibrinolysis. However the magnitude of these effects are modulated by several environmental factors and data will be presented to demonstrate interaction between genotype and presence of ischaemic disease and physical exercise, in the determination of an individual's plasma fibrinogen levels and of triglycerides and diabetes in determining levels of PAI-1.

Published

1997

315. Proton and deuteron structure functions in muon scattering at 470 GeV.

Author

Adams MR, Aïd S, Anthony PL, Averill DA, Baker MD, Baller BR, Banerjee A, Bhatti AA, Bratzler U, Braun HM, Carroll TJ, Clark HL, Conrad JM, Davisson R, Derado I I, Dietrich FS, Dougherty W, Dreyer T, Eckardt V V, Ecker U, Erdmann M, Fang GY, Figiel J, Finlay RW, Gebauer HJ, Geesaman DF, Griffioen KA, Guo RS, Haas J, Halliwell C, Hantke D, Hicks KH, Jackson HE, Jaffe DE, Jancso G, Jansen DM, Jin Z, Kaufman S, Kennedy RD, Kinney ER, Kobrak HG, Kotwal AV, Kunori S, Lord JJ, Lubatti HJ, McLeod D, Madden P, Magill S, Manz A, Melanson H, Michael DG, Montgomery HE, Morfin JG, Nickerson RB, Novak J, O'Day S, Olkiewicz K, Osborne L, Otten R, Papavassiliou V V, Pawlik B, Pipkin FM, Potterveld DH, and Ramberg EJ

Published

1996

316. The acute rise in plasma fibrinogen concentration with exercise is influenced by the G-453-A polymorphism of the beta-fibrinogen gene.

Author

Montgomery HE, Clarkson P, Nwose OM, Mikailidis DP, Jagroop IA, Dollery C, Moult J, Benhizia F, Deanfield J, Jubb M, World M, McEwan JR, Winder A, and Humphries S

Subjects

Adolescent, Adult, Fibrinogen analysis, Genotype, Humans, Male, Exercise, Fibrinogen genetics, Polymorphism, Genetic

Abstract

We have investigated the effects of chronic physical training and acute intensive exercise on plasma fibrinogen levels and the relationship of these responses to beta-fibrinogen G-453-A polymorphism genotype. One hundred fifty-six male British Army recruits were studied at the start of their 10-week basic training, which emphasizes physical fitness. Cohorts were restudied between 0.5 and 5 days after a major 2-day strenuous military exercise (ME) undertaken in their final week of training. Changes in fibrinogen concentration were adjusted for the effects of age, body mass index, and smoking history. Compared with baseline values, fibrinogen concentrations were significantly lower (11.9%, P=.04) at day 5 after ME, consistent with the beneficial effect of training. However, they were higher on days 1 through 3 after ME (suggesting an "acute-phase" response to strenuous exercise) and were maximal on days 1 and 2 (27.2%, P<.001 and 37.1%, P<.001 respectively). Fibrinogen genotype was available in 149 individuals. As expected from previous studies, men with one or more fibrinogen gene A-453 alleles had plasma fibrinogen concentration slightly but significantly higher at baseline (4.5%, P=.11). During the acute-phase response (days 2 and 3), however, the degree of rise was strongly related to the presence of the A allele, being 26.7+/-5.4% (mean+/-SE), 36.5+/-11.0%, and 89.2+/-30.7 for the GG, GA, and AA genotypes, respectively (P=.01). These results confirm that chronic exercise training lowers plasma fibrinogen levels, that intensive exercise generates an acute-phase rise in levels, and that this acute response is strongly influenced by the G/A polymorphism of the beta-fibrinogen gene.

Published

1996

317. Rhabdomyolysis and multiple system organ failure with streptokinase.

Author

Montgomery HE, McIntyre CW, Almond MK, Davies K, Pumphrey CW, and Bennett D

Subjects

Humans, Male, Middle Aged, Myocardial Infarction drug therapy, Fibrinolytic Agents adverse effects, Multiple Organ Failure chemically induced, Rhabdomyolysis chemically induced, Streptokinase adverse effects, Thrombolytic Therapy adverse effects

Published

1995

318. Extraction of the Ratio Fn2/Fp2 from Muon-Deuteron and Muon-Proton Scattering at Small x and Q2.

Author

Adams MR, Aïd S, Anthony PL, Averill DA, Baker MD, Baller BR, Banerjee A, Bhatti AA, Bratzler U, Braun HM, Carroll TJ, Clark HL, Conrad JM, Davisson R, Derado I I, Dhawan SK, Dietrich FS, Dougherty W, Dreyer T, Eckardt V V, Ecker U, Erdmann M, Fang GY, Figiel J, Finlay RW, Gebauer HJ, Geesaman DF, Griffioen KA, Guo RS, Haas J, Halliwell C, Hantke D, Hicks KH, Hughes VW, Jackson HE, Jaffe DE, Jancso G, Jansen DM, Jin Z, Kaufman S, Kennedy RD, Kinney ER, Kobrak HG, Kotwal AV, Kunori S, Lord JJ, Lubatti HJ, McLeod D, Madden P, Magill S, Manz A, Melanson H, Michael DG, Montgomery HE, Morfin JG, Nickerson RB, Novak J, O'Day S, Olkiewicz K, Osborne L, Otten R, Papavassiliou V V, Pawlik B, and Pipkin FM

Published

1995

319. Heparin in unstable angina.

Author

Montgomery HE and Chester MR

Subjects

Drug Therapy, Combination, Female, Heparin administration & dosage, Humans, Infusions, Intravenous, Injections, Subcutaneous, Male, Myocardial Infarction drug therapy, Randomized Controlled Trials as Topic standards, Angina, Unstable drug therapy, Aspirin therapeutic use, Heparin therapeutic use

Published

1995

320. Nuclear decay following deep inelastic scattering of 470 GeV muons.

Author

Adams MR, Aïd S, Anthony PL, Averill DA, Baker MD, Baller BR, Banerjee A, Bhatti AA, Bratzler U, Braun HM, Breidung H, Busza W, Carroll TJ, Clark HL, Conrad JM, Davisson R, Derado I I, Dhawan SK, Dietrich FS, Dougherty W, Dreyer T, Eckardt V V, Ecker U, Erdmann M, Fang GY, Figiel J, Finlay RW, Gebauer HJ, Geesaman DF, Griffioen KA, Guo RS, Haas J, Halliwell C, Hantke D, Hicks KH, Hughes VW, Jackson HE, Jaffe DE, Jancso G, Jansen DM, Jin Z, Kaufman S, Kennedy RD, Kinney ER, Kirk T, Kobrak HG, Kotwal AV, Kunori S, Lord JJ, Lubatti HJ, McLeod D, Madden P, Magill S, Manz A, Melanson H, Michael DG, Montgomery HE, Morfin JG, Nickerson RB, O'Day S, Olkiewicz K, Osborne L, Otten R, and Papavassiliou V V

Published

1995

321. Lack of association between the insertion/deletion polymorphism of the angiotensin-converting enzyme gene and idiopathic dilated cardiomyopathy.

Author

Montgomery HE, Keeling PJ, Goldman JH, Humphries SE, Talmud PJ, and McKenna WJ

Subjects

Adult, Alleles, Case-Control Studies, Disease Progression, Electrophoresis, Agar Gel, Female, Gene Frequency, Genotype, Humans, Incidence, Male, Middle Aged, Polymerase Chain Reaction, Polymorphism, Genetic, Renin-Angiotensin System physiology, Cardiomyopathy, Dilated genetics, Gene Deletion, Peptidyl-Dipeptidase A genetics

Abstract

Objectives: We sought to investigate the role of polymorphisms of the gene for angiotensin-converting enzyme in the development and progression of idiopathic dilated cardiomyopathy., Background: Cardiovascular renin-angiotensin systems may be involved in cardiac remodeling and fibrosis. The absence (deletion [D]) of a 287-base pair marker in the angiotensin-converting enzyme gene (introm 16) is associated with increased serum angiotensin-converting enzyme levels. The DD genotype may be a risk factor for the development of end-stage heart failure due to cardiomyopathy. We therefore examined the relation of the angiotensin-converting enzyme genotype to idiopathic dilated cardiomyopathy and to markers of disease severity., Methods: We studied 364 control subjects and 99 consecutive patients with idiopathic dilated cardiomyopathy. When the incidence of the DD genotype in our control group was assumed to be similar to that previously reported (27%), this study had a power of 0.9 to detect a different incidence in the patient group, if the true incidence in patients was 42%. Deoxyribonucleic acid (DNA) was isolated from blood samples, and angiotensin-converting enzyme genotype was determined by specific polymerase chain reaction and separation of amplified fragments by agarose gel electrophoresis. We also compared genotype distribution with that in previously reported European control subjects. Functional status, clinical course over a mean +/- SD of 28 +/- 33 months and outcome were documented. Cardiac morphology and function and evidence of rhythm disturbance were noninvasively determined., Results: Angiotensin-converting enzyme genotype distribution and allele frequencies were similar in patients and control subjects to within 10% (with 95% confidence) and were also similar between patients and European control subjects. No markers of disease severity or progression other than duration of symptoms before diagnosis and the number of ventricular ectopic beats/h were significantly associated with the presence of the DD alleles., Conclusions: We find no evidence to support an association between angiotensin-converting enzyme genotype and either the diagnosis of idiopathic dilated cardiomyopathy itself or progression of the disease.

Published

1995

322. Measurement of nuclear transparencies from exclusive rho 0 meson production in muon-nucleus scattering at 470 GeV.

Author

Adams MR, Aïd S, Anthony PL, Averill DA, Baker MD, Baller BR, Banerjee A, Bhatti AA, Bratzler U, Braun HM, Breidung H, Busza W, Carroll TJ, Clark HL, Conrad JM, Davisson R, Derado I I, Dhawan SK, Dietrich FS, Dougherty W, Dreyer T, Eckardt V V, Ecker U, Erdmann M, Faller F, Fang GY, Figiel J, Finlay RW, Gebauer HJ, Geesaman DF, Griffioen KA, Guo RS, Haas J, Halliwell C, Hantke D, Hicks KH, Hughes VW, Jackson HE, Jancso G, Jansen DM, Jin Z, Kaufman S, Kennedy RD, Kinney ER, Kirk T, Kobrak HG, Kotwal AV, Kunori S, Lancaster S, Lord JJ, Lubatti HJ, McLeod D, Madden P, Magill S, Manz A, Melanson H, Michael DG, Montgomery HE, Morfin JG, Nickerson RB, O'Day S, Olkiewicz K, Osborne L, and Otten R

Published

1995

323. Scaled energy (z) distributions of charged hadrons observed in deep-inelastic muon scattering at 490 GeV from xenon and deuterium targets.

Author

Adams MR, Aïd S, Anthony PL, Baker MD, Bartlett J, Bhatti AA, Braun HM, Busza W, Carroll T, Conrad JM, Coutrakon G, Davisson R, Derado I I, Dhawan SK, Dougherty W, Dreyer T, Dziunikowska K, Eckardt V V, Ecker U, Erdmann M, Eskreys A, Figiel J, Gebauer HJ, Geesaman DF, Gilman R, Green MC, Haas J, Halliwell C, Hanlon J, Hantke D, Hughes VW, Jackson HE, Jaffe DE, Jancso G, Jansen DM, Kaufman S, Kennedy RD, Kirk T, Kobrak HG, Krzywdzinski S, Kunori S, Lord JJ, Lubatti HJ, McLeod D, Magill S, Malecki P, Manz A, Melanson H, Michael DG, Mohr W, Montgomery HE, Morfin JG, Nickerson RB, O'Day S, Olkiewicz K, Osborne L, Papavassiliou V V, Pawlik B, Pipkin FM, Ramberg EJ, Röser A, Ryan JJ, Salvarani A, and Schellman H

Published

1994

324. Unsuspected coronary artery disease revealed by administration of nebulised salbutamol.

Author

Montgomery HE, Gill J, and Pumphrey CW

Subjects

Adult, Aerosols, Albuterol administration & dosage, Coronary Disease physiopathology, Humans, Male, Albuterol adverse effects, Coronary Disease diagnosis, Electrocardiography drug effects

Published

1994

325. Magnesium and myocardial infarction.

Author

Montgomery HE and Speechly-Dick ME

Subjects

Aspirin therapeutic use, Captopril administration & dosage, Drug Therapy, Combination, Heparin administration & dosage, Humans, Magnesium administration & dosage, Streptokinase administration & dosage, Myocardial Infarction drug therapy

Published

1994

326. Q2 dependence of the average squared transverse energy of jets in deep-inelastic muon-nucleon scattering with comparison to perturbative QCD predictions.

Author

Adams MR, Arndotïd S, Anthony PL, Baker MD, Bartlett J, Bhatti AA, Braun HM, Busza W, Conrad JM, Coutrakon G, Davisson R, Derado I I, Dhawan SK, Dougherty W, Dreyer T, Dziunikowska K, Eckardt V V, Ecker U, Erdmann M, Eskreys A, Figiel J, Gebauer HJ, Geesaman DF, Gilman R, Green MC, Haas J, Halliwell C, Hanlon J, Hantke D, Hughes VW, Jackson HE, Jaffe DE, Jancso G, Jansen DM, Kaufman S, Kennedy RD, Kirk T, Kobrak HG, Krzywdzinski S, Kunori S, Lord JJ, Lubatti HJ, McLeod D, Magill S, Malecki P, Manz A, Melanson H, Michael DG, Mohr W, Montgomery HE, Morfin JG, Nickerson RB, O'Day S, Olkiewicz K, Osborne L, Papavassiliou V V, Pawlik B, Pipkin FM, Ramberg EJ, Röser A, Ryan JJ, Salgado CW, Salvarani A, and Schellman H

Published

1994

327. Perturbative QCD effects observed in 490 GeV deep-inelastic muon scattering.

Author

Adams MR, Aïd S, Anthony PL, Baker MD, Bartlett J, Bhatti AA, Braun HM, Busza W, Conrad JM, Coutrakon G, Davisson R, Derado I I, Dhawan SK, Dougherty W, Dreyer T, Dziunikowska K, Eckardt V V, Ecker U, Erdmann M, Eskreys A, Figiel J, Gebauer HJ, Geesaman DF, Gilman R, Green MC, Haas J, Halliwell C, Hanlon J, Hantke D, Hughes VW, Jackson HE, Jaffe DE, Jancso G, Jansen DM, Kaufman S, Kennedy RD, Kirk T, Kobrak HG, Krzywdzinski S, Kunori S, Lord JJ, Lubatti HJ, McLeod D, Magill S, Malecki P, Manz A, Melanson H, Michael DG, Mohr W, Montgomery HE, Morfin JG, Nickerson RB, O'Day S, Olkiewicz K, Osborne L, Papavassiliou V V, Pawlik B, Pipkin FM, Ramberg EJ, Röser A, Ryan JJ, Salgado CW, Salvarani A, and Schellman H

Published

1993

328. First measurements of jet production rates in deep-inelastic lepton-proton scattering.

Author

Adams MR, Aïd S, Anthony PL, Baker MD, Bartlett J, Bhatti AA, Braun HM, Busza W, Conrad JM, Coutrakon G, Davisson R, Derado I I, Dhawan SK, Dougherty W, Dreyer T, Dziunikowska K, Eckardt V V, Ecker U, Erdmann M, Eskreys A, Figiel J, Gebauer HJ, Geesaman DF, Gilman R, Green MC, Haas J, Halliwell C, Hanlon J, Hantke D, Hughes VW, Jackson HE, Jaffe DE, Jancso G, Jansen DM, Kaufman S, Kennedy RD, Kobrak HG, Krzywdzinski S, Kunori S, Lord JJ, Lubatti HJ, McLeod D, Magill S, Malecki P, Manz A, Michael DG, Mohr W, Montgomery HE, Morfin JG, Nickerson RB, O'Day S, Olkiewicz K, Osborne L, Papavassiliou V V, Pawlik B, Pipkin FM, Ramberg EJ, Röser A, Ryan J, Salgado CW, Salvarani A, Schellman H, Schmitz N, and Schüler KP

Published

1992

329. Saturation of shadowing at very low Bjorken x.

Author

Adams MR, Aïd S, Anthony PL, Baker MD, Bartlett J, Bhatti AA, Braun HM, Busza W, Carroll TJ, Conrad JM, Coutrakon G, Davisson R, Derado I I, Dhawan SK, Dougherty W, Dreyer T, Dziunikowska K, Eckardt V V, Ecker U, Erdmann M, Eskreys A, Figiel J, Gebauer HJ, Geesaman DF, Gilman R, Green MC, Haas J, Halliwell C, Hanlon J, Hantke D, Hughes VW, Jackson HE, Jaffe DE, Jancso G, Jansen DM, Kaufman S, Kennedy RD, Kirk T, Kobrak HG, Krzywdzinski S, Kunori S, Lord JJ, Lubatti HJ, McLeod D, Magill S, Malecki P, Manz A, Melanson H, Michael DG, Mohr W, Montgomery HE, Morfin JG, Nickerson RB, O'Day S, Olkiewicz K, Osborne L, Papavassiliou V V, Pawlik B, Pipkin FM, Ramberg EJ, Röser A, Ryan JJ, Salvarani A, and Schellman H

Published

1992