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2. Bir, iki, ütsch: Verbale Zählkompetenzen von bilingualen und türkischsprachigen Kindern

Author

Böttiger, C, Bräuning, K, Nührenbörger, M, Schwarzkopf, R, Söbbeke, E, Böttiger, C ( C ), Bräuning, K ( K ), Nührenbörger, M ( M ), Schwarzkopf, R ( R ), Söbbeke, E ( E ), Moser Opitz, Elisabeth; https://orcid.org/0000-0002-5243-4770, Böttiger, C, Bräuning, K, Nührenbörger, M, Schwarzkopf, R, Söbbeke, E, Böttiger, C ( C ), Bräuning, K ( K ), Nührenbörger, M ( M ), Schwarzkopf, R ( R ), Söbbeke, E ( E ), and Moser Opitz, Elisabeth; https://orcid.org/0000-0002-5243-4770

Published
2010

7. 4G5G-Polymorphismus des PAI-1-Genes und Restenoserisiko nach koronarer Stentimplantation

Author

Kastrati, Adnan (Prof. Dr.), Theiss, W. (apl. Prof. Dr.), Böttiger, C. (Dr.), Lahn, Christina, Kastrati, Adnan (Prof. Dr.), Theiss, W. (apl. Prof. Dr.), Böttiger, C. (Dr.), and Lahn, Christina

Abstract

In dieser Studie wurde der 4G5G-Polymorphismus des PAI-1 von 1850 Patienten mit koronarer Stentimplantation, bei denen nach 6 Monaten eine angiographische Kontrolluntersuchung erfolgte und das klinische Follow-up über 1 Jahr erhoben wurde, evaluiert. Untersucht wurde, ob der Insertions-Deletions-Polymorphismus in der Promotorregion des PAI-1-Genes einen Einfluss auf die Instent-Restenose hat. Die 4G-Allel-Frequenz betrug 0,56. 32,5 % der für das 4G-Allel homozygoten Patienten entwickelten eine Restenose, im Vergleich dazu 32,2% der Heterozygoten und 35,7 % der Homozygoten für das 5G-Allel (p= 0,52). Dies führt zu der Aussage, dass es keinen signifikanten Unterschied bei den drei Genotypen bezüglich der Ausgangsfragestellung gab. Bezüglich der großen kardialen Ereignisse war das frühe Outcome sowie das Outcome nach einem Jahr mit 5,6 % beim 4G4G-Genotyp, 5,3% beim 4G5G-Genotyp und 4,6 % beim 5G5G-Genotyp nicht signifikant abhängig vom Genotyp. Als Schlussfolgerung ergibt sich daher, dass dem 4G5G-Polymorphismus von PAI-1 keine Rolle bei der Entwicklung einer Restenose nach koronarer Stentimplantation zugeschrieben werden kann., Plasinogen activator inhibitor-1 has been proposed as a candidate risk factor for restenosis after coronary artery stenting. Transcription, level, and activity of PAI-1 are influenced by the 4G/5G polymorphism in the promotor region of PAI-1 gene. The polymorphism may therefore affect wound.healing processes in injured blood vessels and influence restenosis. In 1850 consecutive patients, angiographic measures of restenosis and the clinical outcome at 30 days and 1 year after stent implantation were evaluated. Angiographic restenosis was defined as >50% diameter restenosis determined at follow-up angiography, performed 6 months after stenting. The 4G/5G genotypes were determined with TaqMan technique. Among the patients, the frequency of the 4G allele was 0.55. Follow-up angiography was done in 84% of the patients. We observed restenosis in 32.5% of the 4G/4G carriers, 32.2% of the 4G/5G carriers, and 35.7% of the 5G/5G carriers (P= .52). The occurrence of a major adverse event (death, myocardial infarction, or target vessel revascularization due to restenosis-induced ischemia) was in 5.6% in 4G/5G carriers, 5.3% in 4G/5G carriers, and 4.6% in 5G/5G carriers in 30 days (P= .80), and 24.7% in 4G/4G carriers, 23.0% in 4G/5G carriers, and 26.2% in 5G/5G carriers at 1 year (P= . 45). The 4G/5G polymorphism of the PAI-1 gene is not associated with an increased risk of thrombotic and restenotic events after coronary artery stenting.

Published
2005

8. 4G5G-Polymorphismus des PAI-1-Genes und Restenoserisiko nach koronarer Stentimplantation

Author

Böttiger, C. (Dr.), Kastrati, Adnan (Prof. Dr.);Theiss, W. (apl. Prof. Dr.), Lahn, Christina, Böttiger, C. (Dr.), Kastrati, Adnan (Prof. Dr.);Theiss, W. (apl. Prof. Dr.), and Lahn, Christina

Abstract

In dieser Studie wurde der 4G5G-Polymorphismus des PAI-1 von 1850 Patienten mit koronarer Stentimplantation, bei denen nach 6 Monaten eine angiographische Kontrolluntersuchung erfolgte und das klinische Follow-up über 1 Jahr erhoben wurde, evaluiert. Untersucht wurde, ob der Insertions-Deletions-Polymorphismus in der Promotorregion des PAI-1-Genes einen Einfluss auf die Instent-Restenose hat. Die 4G-Allel-Frequenz betrug 0,56. 32,5 % der für das 4G-Allel homozygoten Patienten entwickelten eine Restenose, im Vergleich dazu 32,2% der Heterozygoten und 35,7 % der Homozygoten für das 5G-Allel (p= 0,52). Dies führt zu der Aussage, dass es keinen signifikanten Unterschied bei den drei Genotypen bezüglich der Ausgangsfragestellung gab. Bezüglich der großen kardialen Ereignisse war das frühe Outcome sowie das Outcome nach einem Jahr mit 5,6 % beim 4G4G-Genotyp, 5,3% beim 4G5G-Genotyp und 4,6 % beim 5G5G-Genotyp nicht signifikant abhängig vom Genotyp. Als Schlussfolgerung ergibt sich daher, dass dem 4G5G-Polymorphismus von PAI-1 keine Rolle bei der Entwicklung einer Restenose nach koronarer Stentimplantation zugeschrieben werden kann., Plasinogen activator inhibitor-1 has been proposed as a candidate risk factor for restenosis after coronary artery stenting. Transcription, level, and activity of PAI-1 are influenced by the 4G/5G polymorphism in the promotor region of PAI-1 gene. The polymorphism may therefore affect wound.healing processes in injured blood vessels and influence restenosis. In 1850 consecutive patients, angiographic measures of restenosis and the clinical outcome at 30 days and 1 year after stent implantation were evaluated. Angiographic restenosis was defined as >50% diameter restenosis determined at follow-up angiography, performed 6 months after stenting. The 4G/5G genotypes were determined with TaqMan technique. Among the patients, the frequency of the 4G allele was 0.55. Follow-up angiography was done in 84% of the patients. We observed restenosis in 32.5% of the 4G/4G carriers, 32.2% of the 4G/5G carriers, and 35.7% of the 5G/5G carriers (P= .52). The occurrence of a major adverse event (death, myocardial infarction, or target vessel revascularization due to restenosis-induced ischemia) was in 5.6% in 4G/5G carriers, 5.3% in 4G/5G carriers, and 4.6% in 5G/5G carriers in 30 days (P= .80), and 24.7% in 4G/4G carriers, 23.0% in 4G/5G carriers, and 26.2% in 5G/5G carriers at 1 year (P= . 45). The 4G/5G polymorphism of the PAI-1 gene is not associated with an increased risk of thrombotic and restenotic events after coronary artery stenting.

Published
2005

10. Angiotensin I-converting enzyme (ACE) inhibitors and restenosis after coronary artery stenting in patients with the DD genotype of the ACE gene.

Author

Koch W, Mehilli J, von Beckerath N, Böttiger C, Schömig A, Kastrati A, Koch, Werner, Mehilli, Julinda, von Beckerath, Nicolas, Böttiger, Corinna, Schömig, Albert, and Kastrati, Adnan

Abstract

Objectives: We tested the hypothesis that patients with the DD genotype of the angiotensin I-converting enzyme (ACE) gene who are treated with ACE inhibitors are at a higher risk of restenosis after coronary stent placement than patients who do not receive ACE inhibitors.Background: Two recent studies with a limited series of patients carrying the DD genotype suggested an unfavorable impact of the use of ACE inhibitors on the restenotic process after implantation of stents in coronary arteries. Because these findings may question the use of ACE inhibitors after coronary stenting, we examined this important issue in a large series of patients.Methods: We determined the ACE gene I/D genotype of 2,222 consecutive patients with symptomatic coronary artery disease who underwent stent implantation. The patients with the DD genotype (n = 612) constituted the study population. The primary end point was in-stent restenosis, which was assessed as angiographic restenosis (> or =50% diameter stenosis at six-month follow-up) and clinical restenosis (need for target vessel revascularization due to symptoms or signs of ischemia in the presence of angiographic restenosis over one year after the intervention).Results: Of the 612 patients with the DD genotype, 403 (65.8%) were treated with ACE inhibitors and 209 (34.2%) did not receive ACE inhibitors. The angiographic and clinical restenosis rates were not significantly different between the group treated with ACE inhibitors and the group not receiving ACE inhibitors (p = 0.55). Continuous measures of restenosis, minimal lumen diameter, diameter stenosis, late lumen loss, and loss index were also similar in both groups (p > or = 0.55). In addition, one-year survival free of myocardial infarction was not significantly different between the two groups (p = 0.27).Conclusions: In contrast to previous reports, our study provides evidence that patients carrying the DD genotype are not exposed to an increased risk of restenosis after stent placement when treated with ACE inhibitors. [ABSTRACT FROM AUTHOR]

Published
2003
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11. Association of a CD18 gene polymorphism with a reduced risk of restenosis after coronary stenting.

Author

Koch, Werner, Böttiger, Corrina, Mehilli, Julinda, von Beckerath, Nicolas, Neumann, Franz-Josef, Schömig, Albert, Kastrati, Adnan, Koch, W, Böttiger, C, Mehilli, J, von Beckerath, N, Neumann, F J, Schömig, A, and Kastrati, A

Subjects
*HEART diseases, *CARDIOLOGY
Abstract

Inflammatory mechanisms play an important role in the process of restenosis after percutaneous coronary interventions, with cell adhesion molecules, including Mac-1 (CD11b/CD18), as key mediators. A single nucleotide polymorphism, 1323C/T, located in exon 11 of the CD18 gene has been previously described, but its functional and clinical significances have not yet been studied. We assessed whether an association exists between this polymorphism and restenosis after coronary stenting. Clinical and angiographic measures of restenosis were evaluated over 1 year after coronary stent placement in 1,207 consecutive patients. Angiographic restenosis was defined as a > or =50% diameter stenosis at follow-up angiography. Determination of the CD18 1323C/T genotype was based on the polymerase chain reaction technique. The frequency of the T allele was 0.34 and its presence reduced the 1-year risk of a major adverse cardiac event (death, myocardial infarction, target vessel revascularization) by 29% (p = 0.011). Carriers of the T allele had a significantly lower risk of angiographic restenosis compared with noncarriers (odds ratio 0.71, 95% confidence interval 0.55 to 0.92). The incidence of restenosis decreased as a function of the number of T alleles: 38.1% in patients with genotype CC, 31.7% in patients with genotype CT, and 26.0% in patients with genotype TT (p = 0.004). Thus, the 1323T allele of the CD18 gene is associated, in a gene dose-dependent manner, with a lower incidence of angiographic restenosis after coronary stenting. This finding suggests that Mac-1 is involved in the development of restenosis after coronary stent placement. [ABSTRACT FROM AUTHOR]

Published
2001
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13. 4G5G-Polymorphismus des PAI-1-Genes und Restenoserisiko nach koronarer Stentimplantation

Author

Lahn, Christina, Böttiger, C. (Dr.), Kastrati, Adnan (Prof. Dr.), and Theiss, W. (apl. Prof. Dr.)

Subjects
4G/5G polmorphism, PAI-1 gene, restenosis, Medizin, ddc:610, 4G/5G-Polymorphismus, PAI-1, Restenose
Abstract

In dieser Studie wurde der 4G5G-Polymorphismus des PAI-1 von 1850 Patienten mit koronarer Stentimplantation, bei denen nach 6 Monaten eine angiographische Kontrolluntersuchung erfolgte und das klinische Follow-up über 1 Jahr erhoben wurde, evaluiert. Untersucht wurde, ob der Insertions-Deletions-Polymorphismus in der Promotorregion des PAI-1-Genes einen Einfluss auf die Instent-Restenose hat. Die 4G-Allel-Frequenz betrug 0,56. 32,5 % der für das 4G-Allel homozygoten Patienten entwickelten eine Restenose, im Vergleich dazu 32,2% der Heterozygoten und 35,7 % der Homozygoten für das 5G-Allel (p= 0,52). Dies führt zu der Aussage, dass es keinen signifikanten Unterschied bei den drei Genotypen bezüglich der Ausgangsfragestellung gab. Bezüglich der großen kardialen Ereignisse war das frühe Outcome sowie das Outcome nach einem Jahr mit 5,6 % beim 4G4G-Genotyp, 5,3% beim 4G5G-Genotyp und 4,6 % beim 5G5G-Genotyp nicht signifikant abhängig vom Genotyp. Als Schlussfolgerung ergibt sich daher, dass dem 4G5G-Polymorphismus von PAI-1 keine Rolle bei der Entwicklung einer Restenose nach koronarer Stentimplantation zugeschrieben werden kann. Plasinogen activator inhibitor-1 has been proposed as a candidate risk factor for restenosis after coronary artery stenting. Transcription, level, and activity of PAI-1 are influenced by the 4G/5G polymorphism in the promotor region of PAI-1 gene. The polymorphism may therefore affect wound.healing processes in injured blood vessels and influence restenosis. In 1850 consecutive patients, angiographic measures of restenosis and the clinical outcome at 30 days and 1 year after stent implantation were evaluated. Angiographic restenosis was defined as >50% diameter restenosis determined at follow-up angiography, performed 6 months after stenting. The 4G/5G genotypes were determined with TaqMan technique. Among the patients, the frequency of the 4G allele was 0.55. Follow-up angiography was done in 84% of the patients. We observed restenosis in 32.5% of the 4G/4G carriers, 32.2% of the 4G/5G carriers, and 35.7% of the 5G/5G carriers (P= .52). The occurrence of a major adverse event (death, myocardial infarction, or target vessel revascularization due to restenosis-induced ischemia) was in 5.6% in 4G/5G carriers, 5.3% in 4G/5G carriers, and 4.6% in 5G/5G carriers in 30 days (P= .80), and 24.7% in 4G/4G carriers, 23.0% in 4G/5G carriers, and 26.2% in 5G/5G carriers at 1 year (P= . 45). The 4G/5G polymorphism of the PAI-1 gene is not associated with an increased risk of thrombotic and restenotic events after coronary artery stenting.

Published
2005

14. Comparison of vascular closure devices vs manual compression after femoral artery puncture: the ISAR-CLOSURE randomized clinical trial.

Author

Schulz-Schüpke S, Helde S, Gewalt S, Ibrahim T, Linhardt M, Haas K, Hoppe K, Böttiger C, Groha P, Bradaric C, Schmidt R, Bott-Flügel L, Ott I, Goedel J, Byrne RA, Schneider S, Burgdorf C, Morath T, Kufner S, Joner M, Cassese S, Hoppmann P, Hengstenberg C, Pache J, Fusaro M, Massberg S, Mehilli J, Schunkert H, Laugwitz KL, and Kastrati A

Subjects
Aged, Cardiac Catheterization, Coronary Angiography methods, Female, Femoral Artery, Hemostasis, Humans, Male, Middle Aged, Punctures, Time Factors, Coronary Angiography adverse effects, Hemostatic Techniques, Pressure, Vascular Closure Devices
Abstract

Importance: The role of vascular closure devices (VCD) for the achievement of hemostasis in patients undergoing transfemoral coronary angiography remains controversial., Objective: To compare outcomes with the use of 2 hemostasis strategies after diagnostic coronary angiography performed via transfemoral access-a VCD-based strategy with 2 types of devices, an intravascular device and an extravascular device, vs standard manual compression. The primary hypothesis to be tested was that femoral hemostasis achieved through VCD is noninferior to manual compression in terms of vascular access-site complications. A secondary objective was the comparison of the 2 types of VCD., Design, Setting, and Participants: Randomized, large-scale, multicenter, open-label clinical trial. We enrolled 4524 patients undergoing coronary angiography with a 6 French sheath via the common femoral artery from April 2011 through May 2014 in 4 centers in Germany. Last 30-day follow-up was performed in July 2014., Interventions: After angiography of the access site, patients were randomized to hemostasis with an intravascular VCD, extravascular VCD, or manual compression in a 1:1:1 ratio., Main Outcomes and Measures: Primary end point: the composite of access site-related vascular complications at 30 days after randomization with a 2% noninferiority margin. Secondary end points: time to hemostasis, repeat manual compression, and VCD failure. An α-level of .025 was chosen for primary and secondary comparisons., Results: Of the 4524 enrolled patients, 3015 were randomly assigned to a VCD group (1509 received intravascular VCD and 1506 received extravascular VCD) and 1509 patients were randomly assigned to the manual compression group. Before hospital discharge, duplex sonography of the access site was performed in 4231 (94%) patients. The primary end point was observed in 208 patients (6.9%) assigned to receive a VCD and 119 patients (7.9%) assigned to manual compression (difference, -1.0% [1-sided 97.5% CI, 0.7%]; P for noninferiority<.001). Time to hemostasis was significantly shorter in patients with VCD (1 minute [interquartile range {IQR}, 0.5-2.0]), vs manual compression (10 minutes [IQR, 10-15]; P < .001). Time to hemostasis was significantly shorter among patients with intravascular VCD (0.5 minute [IQR, 0.2-1.0]), vs extravascular VCD (2.0 minutes [IQR, 1.0-2.0]; P <.001) and closure device failure was also significantly lower among those with intravascular vs extravascular VCD (80 patients [5.3%], vs 184 patients [12.2%]; P < .001)., Conclusions and Relevance: In patients undergoing transfemoral coronary angiography, VCDs were noninferior to manual compression in terms of vascular access-site complications and reduced time to hemostasis., Trial Registration: clinicaltrials.gov Identifier: NCT01389375.

Published
2014
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15. Rationale and design of a randomised clinical trial comparing vascular closure device and manual compression to achieve haemostasis after diagnostic coronary angiography: the Instrumental Sealing of ARterial puncture site - CLOSURE device versus manual compression (ISAR-CLOSURE) trial.

Author

Xhepa E, Byrne RA, Schulz S, Helde S, Gewalt S, Cassese S, Linhardt M, Ibrahim T, Mehilli J, Hoppe K, Grupp K, Kufner S, Böttiger C, Hoppmann P, Burgdorf C, Fusaro M, Ott I, Schneider S, Hengstenberg C, Schunkert H, Laugwitz KL, and Kastrati A

Subjects
Clinical Protocols, Equipment Design, Germany, Hemorrhage blood, Hemorrhage etiology, Hemostatic Techniques adverse effects, Humans, Pressure, Prospective Studies, Punctures, Time Factors, Treatment Outcome, Coronary Angiography adverse effects, Femoral Artery, Hemorrhage prevention & control, Hemostasis, Hemostatic Techniques instrumentation, Research Design, Vascular Access Devices
Abstract

Aims: Vascular closure devices (VCD) have been introduced into clinical practice with the aim of increasing the procedural efficiency and clinical safety of coronary angiography. However, clinical studies comparing VCD and manual compression have yielded mixed results, and large randomised clinical trials comparing the two strategies are missing. Moreover, comparative efficacy studies between different VCD in routine clinical use are lacking., Methods and Results: The Instrumental Sealing of ARterial puncture site - CLOSURE device versus manual compression (ISAR-CLOSURE) trial is a prospective, randomised clinical trial designed to compare the outcomes associated with the use of VCD or manual compression to achieve femoral haemostasis. The test hypothesis is that femoral haemostasis after coronary angiography achieved using VCD is not inferior to manual compression in terms of access-site-related vascular complications. Patients undergoing coronary angiography via the common femoral artery will be randomised in a 1:1:1 fashion to receive FemoSeal VCD, EXOSEAL VCD or manual compression. The primary endpoint is the incidence of the composite of arterial access-related complications (haematoma ≥5 cm, pseudoaneurysm, arteriovenous fistula, access-site-related bleeding, acute ipsilateral leg ischaemia, the need for vascular surgical/interventional treatment or documented local infection) at 30 days after randomisation. According to power calculations based on non-inferiority hypothesis testing, enrolment of 4,500 patients is planned. The trial is registered at www.clinicaltrials.gov (study identifier: NCT01389375)., Conclusions: The safety of VCD as compared to manual compression in patients undergoing transfemoral coronary angiography remains an issue of clinical equipoise. The aim of the ISAR-CLOSURE trial is to assess whether femoral haemostasis achieved through the use of VCD is non-inferior to manual compression in terms of access-site-related vascular complications.

Published
2014
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16. Safety and efficacy of a potential treatment algorithm by using manual compression repair and ultrasound-guided thrombin injection for the management of iatrogenic femoral artery pseudoaneurysm in a large patient cohort.

Author

Dzijan-Horn M, Langwieser N, Groha P, Bradaric C, Linhardt M, Böttiger C, Byrne RA, Steppich B, Koppara T, Gödel J, Hadamitzky M, Ott I, von Beckerath N, Kastrati A, Laugwitz KL, and Ibrahim T

Subjects
Aged, Aged, 80 and over, Aneurysm, False diagnostic imaging, Aneurysm, False epidemiology, Cardiac Catheterization adverse effects, Cohort Studies, Combined Modality Therapy, Female, Follow-Up Studies, Humans, Incidence, Injections, Intra-Arterial, Male, Mass Screening, Middle Aged, Musculoskeletal Manipulations adverse effects, Retrospective Studies, Thrombin administration & dosage, Treatment Outcome, Ultrasonography, Interventional adverse effects, Algorithms, Aneurysm, False therapy, Femoral Artery diagnostic imaging, Iatrogenic Disease, Musculoskeletal Manipulations methods, Thrombin therapeutic use, Ultrasonography, Interventional methods
Abstract

Background: Because of the risk of associated complications, femoral pseudoaneurysm (PSA) formation implies further treatment. Ultrasound-guided thrombin injection (UGTI) is becoming the accepted gold standard, but manual compression (MC) represents an established treatment option including PSAs not feasible for UGTI. This study aims to assess our experience in PSA treatment using MC or UGTI according to a potential algorithm based on morphological properties in a large patient cohort., Methods and Results: Between January 2007 and January 2011, a total of 432 PSAs were diagnosed in 29091 consecutive patients (1.49%) undergoing femoral artery catheterization. When compressible, small PSAs (<20 mm), PSAs without clearly definable neck, PSAs directly adjacent to vessels, and PSAs with concomitant arteriovenous fistula were referred to MC (n=145, 34%). All other PSAs were treated by UGTI (n=287, 66%). Follow-up duplex scans were performed within 12 to 14 hours after manual compression therapy and within 4 to 6 hours after UGTI or by the next morning and were available for 428 patients (99.1%). The overall success rate of our institutional therapeutic approach was 97.2%, which was achieved by 178 MC- and 357 UGTI-procedures, respectively. Procedural complications occurred in 5 cases (1.4%) after UGTI and in 3 cases (1.7%) after MC, respectively. The treatment algorithm was not successful in 12 patients, whereas 2 PSAs (0.5%) were successfully excluded by implantation of a covered stent-graft, and 10 patients necessitated surgical intervention (2.3%), which was associated with a high complication rate (30%)., Conclusions: The presented treatment algorithm facilitates effective and safe PSA elimination.

Published
2014
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17. Safety and mid-term outcome of endovascular therapy for internal carotid artery disease: a 15-year experience at a single-centre angiology institution.

Author

Ibrahim T, Karmann S, Schuster T, Fusaro M, Ott I, Böttiger C, Paschalidis M, Hilger JK, Poppert H, Theiss W, and von Beckerath N

Subjects
Age Factors, Aged, Carotid Artery Diseases complications, Carotid Artery Diseases mortality, Disease-Free Survival, Embolic Protection Devices, Female, Germany, Humans, Ischemic Attack, Transient etiology, Kaplan-Meier Estimate, Male, Middle Aged, Multivariate Analysis, Proportional Hazards Models, Recurrence, Retrospective Studies, Risk Factors, Stents, Stroke etiology, Time Factors, Treatment Outcome, Angioplasty, Balloon adverse effects, Angioplasty, Balloon instrumentation, Angioplasty, Balloon mortality, Carotid Artery Diseases therapy, Carotid Artery, Internal
Abstract

Background: Endovascular therapy of carotid artery disease has emerged as a potential alternative to endarterectomy and its clinical practise dramatically increased in many parts of the world. This study aims to determine the safety and mid-term outcome of carotid artery stenting (CAS) within a 15-year carotid program at a single-centre institution., Patients and Methods: We retrospectively analysed all CAS-procedures performed at our institution between 1995 and 2009., Results: During the observation period, a total of 497 CAS procedures were attempted in 460 patients with stenoses of the internal carotid artery of which 187 (37.6 %) were symptomatic and 310 (62.4 %) were asymptomatic. CAS was successful in 479 (96.4 %) cases and success rate significantly increased throughout the study (p < 0.001). The periprocedural complication rate for death, stroke, and transient ischemic attack (TIA) was 0.4 %, 1.2 %, and 2.6 %, respectively, and the cumulative event rate did not differ between symptomatic and asymptomatic patients (4.8 % vs. 3.9 %; p = 0.62). Age was the only significant predictor for the occurrence of any periprocedural adverse event (OR 2.08 [1.22 - 3.54]; p = 0.007). During a median follow-up of 24 [1; 141] months, the rate of stroke, TIA, and in-stent restenosis was 1.0 %, 2.2 %, and 2.7 %, respectively., Conclusions: Data from this large observation in everyday clinical patients demonstrate that endovascular therapy in carotid artery disease can be performed safely and with mid-term outcomes comparable to carotid endarterectomy.

Published
2013
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18. Pathophysiological interference with neurovascular coupling - when imaging based on hemoglobin might go blind.

Author

Lindauer U, Dirnagl U, Füchtemeier M, Böttiger C, Offenhauser N, Leithner C, and Royl G

Abstract

Assessing neuronal activity by non-invasive functional brain imaging techniques which are based on the hemodynamic response depends totally on the physiological cascade of metabolism and blood flow. At present, functional brain imaging with near infrared spectroscopy (NIRS) or BOLD-fMRI is widely used in cognitive neuroscience in healthy subjects where neurovascular coupling and cerebrovascular reactivity can be assumed to be intact. Local activation studies as well as studies investigating functional connectivity between brain regions of the resting brain provide a rapidly increasing body of knowledge on brain function in humans and animals. Furthermore, functional NIRS and MRI techniques are increasingly being used in patients with severe brain diseases and this use might gain more and more importance for establishing their use in the clinical routine. However, more and more experimental evidence shows that changes in baseline physiological parameters, pharmacological interventions, or disease-related vascular changes may significantly alter the normal response of blood flow and blood oxygenation and thus may lead to misinterpretation of neuronal activity. In this article we present examples of recent experimental findings on pathophysiological changes of neurovascular coupling parameters in animals and discuss their potential implications for functional imaging based on hemodynamic signals such as fNIRS or BOLD-fMRI. To enable correct interpretation of neuronal activity by vascular signals, future research needs to deepen our understanding of the basic mechanisms of neurovascular coupling and the specific characteristics of disturbed neurovascular coupling in the diseased brain.

Published
2010
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19. Myosin va mediates docking of secretory granules at the plasma membrane.

Author

Desnos C, Huet S, Fanget I, Chapuis C, Böttiger C, Racine V, Sibarita JB, Henry JP, and Darchen F

Subjects
Cells, Cultured, Humans, Transport Vesicles physiology, Cell Membrane physiology, Myosin Heavy Chains physiology, Myosin Type V physiology, Secretory Vesicles physiology
Abstract

Myosin Va (MyoVa) is a prime candidate for controlling actin-based organelle motion in neurons and neuroendocrine cells. Its function in secretory granule (SG) trafficking was investigated in enterochromaffin cells by wide-field and total internal reflection fluorescence microscopy. The distribution of endogenous MyoVa partially overlapped with SGs and microtubules. Impairing MyoVa function by means of a truncated construct (MyoVa tail) or RNA interference prevented the formation of SG-rich regions at the cell periphery and reduced SG density in the subplasmalemmal region. Individual SG trajectories were tracked to analyze SG mobility. A wide distribution of their diffusion coefficient, D(xy), was observed. Almost immobile SGs (D(xy) < 5 x 10(-4) microm2 x s(-1)) were considered as docked at the plasma membrane based on two properties: (1) SGs that undergo exocytosis have a D(xy) below this threshold value for at least 2 s before fusion; (2) a negative autocorrelation of the vertical motion was found in subtrajectories with a D(xy) below the threshold. Using this criterion of docking, we found that the main effect of MyoVa inhibition was to reduce the number of docked granules, leading to reduced secretory responses. Surprisingly, this reduction was not attributable to a decreased transport of SGs toward release sites. In contrast, MyoVa silencing reduced the occurrence of long-lasting, but not short-lasting, docking periods. We thus propose that, despite its known motor activity, MyoVa directly mediates stable attachment of SGs at the plasma membrane.

Published
2007
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20. 4G/5G polymorphism of the plasminogen activator inhibitor-1 gene and risk of restenosis after coronary artery stenting.

Author

Böttiger C, Koch W, Lahn C, Mehilli J, von Beckerath N, Schömig A, and Kastrati A

Subjects
Coronary Angiography, Coronary Restenosis diagnostic imaging, Female, Follow-Up Studies, Genotype, Germany epidemiology, Humans, Male, Middle Aged, Promoter Regions, Genetic genetics, Survival Rate, Treatment Outcome, Coronary Disease therapy, Coronary Restenosis epidemiology, Coronary Restenosis genetics, Plasminogen Activator Inhibitor 1 genetics, Polymorphism, Genetic, Stents statistics & numerical data, Wound Healing genetics
Abstract

Background: Plasminogen activator inhibitor-1 (PAI-1) has been proposed as a candidate risk factor for restenosis after coronary artery stenting. Transcription, level, and activity of PAI-1 are influenced by the 4G/5G polymorphism in the promoter region of PAI-1 gene. The polymorphism may therefore affect wound-healing processes in injured blood vessels and influence restenosis., Methods: In 1850 consecutive patients, angiographic measures of restenosis and the clinical outcome at 30 days and 1 year after stent implantation were evaluated. Angiographic restenosis was defined as > or =50% diameter stenosis determined at follow-up angiography, performed 6 months after stenting. The 4G/5G genotypes were determined with TaqMan technique., Results: Among the patients, the frequency of the 4G allele was 0.55. Follow-up angiography was done in 84% of the patients. We observed restenosis in 32.5% of 4G/4G carriers, 32.2% of 4G/5G carriers, and 35.7% of 5G/5G carriers (P =.52). The occurrence of a major adverse event (death, myocardial infarction, or target vessel revascularization due to restenosis-induced ischemia) was 5.6% in 4G/4G carriers, 5.3% in 4G/5G carriers, and 4.6% in 5G/5G carriers at 30 days (P =.80), and 24.7% in 4G/4G carriers, 23.0% in 4G/5G carriers, and 26.2% in 5G/5G carriers at 1 year (P =.45)., Conclusion: The 4G/5G polymorphism of the PAI-1 gene is not associated with an increased risk of thrombotic and restenotic events after coronary artery stenting.

Published
2003
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21. Interleukin-10 and tumor necrosis factor gene polymorphisms and risk of coronary artery disease and myocardial infarction.

Author

Koch W, Kastrati A, Böttiger C, Mehilli J, von Beckerath N, and Schömig A

Subjects
Female, Gene Frequency, Genotype, Humans, Linkage Disequilibrium, Male, Middle Aged, Risk Factors, Coronary Disease genetics, Interleukin-10 genetics, Lymphotoxin-alpha genetics, Myocardial Infarction genetics, Polymorphism, Genetic, Tumor Necrosis Factor-alpha genetics
Abstract

Inflammation plays an important role in the pathogenesis of atherosclerosis and acute coronary syndromes. Cytokines IL-10 and TNF-alpha exert opposite functions in inflammatory reactions, IL-10 acting predominantly as an antiinflammatory and TNF-alpha as a proinflammatory factor. Functional single nucleotide polymorphisms in the genes of IL-10, TNF-alpha, and TNF-beta are associated with gene expression and plasma levels of IL-10 and TNF-alpha. The aim of the study was to assess whether these IL-10 and TNF gene polymorphisms are related to the risk of coronary artery disease (CAD) and myocardial infarction (MI). Consecutive, angiographically examined patients with significant coronary stenoses but without symptoms or signs of old or acute MI constituted the group with CAD (n=998) and patients with old or acute MI constituted the group with MI (n=793). Subjects with neither angiographic CAD nor symptoms or signs of MI (n=340) served as controls. They were matched with the patients for age and sex. Genotyping was performed with techniques based on the polymerase chain reaction. Allele frequencies, genotype distributions, and frequencies of allele combinations for three IL-10 promoter polymorphisms, -1082G/A, -819C/T and -592C/A, were similar between CAD patients, MI patients, and matched controls. Similarly, genetic analysis did not reveal group-specific differences for the TNF-alpha promoter polymorphisms -863C/A and -308G/A, as well as for the TNF-beta intron 1 polymorphism 252G/A. In addition, no relationship was found between specific combinations of IL-10 and TNF alleles, indicative of low IL-10 and high TNF-alpha production, respectively, and CAD or MI. The lack of association persisted also after adjusting for other cardiovascular risk factors. Our findings suggest that six different and functionally relevant polymorphisms of the genes coding for IL-10, TNF-alpha, and TNF-beta are neither separately nor in cooperation associated with the risk of CAD or MI in angiographically examined patients.

Published
2001
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22. Glycoprotein Ia C807T polymorphism and risk of restenosis following coronary stenting.

Author

von Beckerath N, Koch W, Mehilli J, Böttiger C, Braun S, Schömig A, and Kastrati A

Subjects
Aged, Base Sequence, Confidence Intervals, Coronary Angiography, Coronary Disease diagnosis, Female, Genetic Markers, Genotype, Humans, Male, Middle Aged, Molecular Sequence Data, Odds Ratio, Polymerase Chain Reaction, Predictive Value of Tests, Probability, Prognosis, Prospective Studies, Receptors, Collagen, Recurrence, Risk Assessment, Risk Factors, Sensitivity and Specificity, Severity of Illness Index, Coronary Disease genetics, Coronary Disease therapy, Integrins genetics, Platelet Adhesiveness genetics, Polymorphism, Genetic, Stents adverse effects
Abstract

Platelets are thought to contribute to development of restenosis following percutaneous coronary interventions. The glycoprotein Ia/IIa complex is a major platelet collagen receptor, its surface expression being influenced by two, linked single nucleotide polymorphisms (C807T and G873A) in the glycoprotein Ia gene. T807 is associated with increased expression of this integrin receptor. We assessed whether T807 is associated with an increased risk of restenosis in 1769 consecutive patients treated with coronary stenting. 6-month follow-up angiograms were available in 82.4% of the patients. C807T genotype distribution was CC in 35.8%, CT in 47.6% and TT in 16.6% of the patients. Restenosis (diameter stenosis > or =50% at follow-up angiography) occurred in 32.9% of CC, 31.5% of CT and 32.1% of TT patients (P=0.87). The rate of major adverse cardiac events (death, myocardial infarction or need of reintervention) within 1 yr was 21.6% for CC, 21.7% for CT and 21.2% for TT patients (P=0.98). Thus, carriage of the GP Ia T807 allele is not associated with an increased risk of restenosis or unfavorable late outcome following coronary artery stenting.

Published
2001
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23. Protective role against restenosis from an interleukin-1 receptor antagonist gene polymorphism in patients treated with coronary stenting.

Author

Kastrati A, Koch W, Berger PB, Mehilli J, Stephenson K, Neumann FJ, von Beckerath N, Böttiger C, Duff GW, and Schömig A

Subjects
Aged, Coronary Disease physiopathology, Female, Humans, Interleukin 1 Receptor Antagonist Protein, Male, Middle Aged, Polymorphism, Genetic, Receptors, Interleukin-1 genetics, Recurrence, Sialoglycoproteins genetics, Coronary Disease therapy, Receptors, Interleukin-1 antagonists & inhibitors, Sialoglycoproteins pharmacology, Stents
Abstract

Objectives: To test the hypothesis that interleukin-1 receptor antagonist (IL-1ra) gene polymorphism contributes to the risk of restenosis after coronary stenting., Background: Cytokines of the interleukin-1 (IL-1) family play a central role in regulating inflammatory responses. There is strong evidence to support IL-1 involvement in smooth muscle cell mitogenesis and extracellular matrix metabolism. The IL-1ra counters the proinflammatory effects of IL-1. The interleukin-1 receptor antagonist gene (IL-1RN) contains several well-characterized polymorphic sites that correlate with altered IL-lra levels., Methods: In 1,850 consecutive patients, clinical and angiographic measures ofrestenosis were evaluated over one year after coronary stent placement. Repeat angiography at six months was achieved in 84% of the patients; angiographic restenosis was defined < or =50% diameter stenosis at follow-up. Genotyping for an exon 2 polymorphism (+2,018) of IL-1RN (alleles 1 and 2) was based on a polymerase chain reaction technique., Results: Allele 2 frequency was 0.28. Carriers of allele 2 had a significantly lower risk for angiographic restenosis, odds ratio (OR) of 0.78 (95% confidence interval, 0.63 to 0.97) and target vessel revascularization, OR of 0.73 (0.58 to 0.92) compared with noncarriers. Risk reduction was especially significant in patients <60 years (n = 696), with OR of 0.63 (0.43 to 0.91) for angiographic restenosis and 0.55 (0.39 to 0.78) for target vessel revascularization., Conclusions: Allele 2 of the IL-1ra gene was associated with a lower incidence of restenosis after coronary stenting, particularly in younger patients. This finding supports a role of inflammation in the development of restenosis after stent placement.

Published
2000
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24. Insertion/deletion polymorphism of the angiotensin I-converting enzyme gene is not associated with restenosis after coronary stent placement.

Author

Koch W, Kastrati A, Mehilli J, Böttiger C, von Beckerath N, and Schömig A

Subjects
Aged, Constriction, Pathologic, Coronary Angiography, Coronary Disease epidemiology, Coronary Disease genetics, Coronary Disease surgery, Coronary Thrombosis epidemiology, Coronary Thrombosis surgery, Female, Follow-Up Studies, Genetic Predisposition to Disease, Genotype, Humans, Male, Middle Aged, Myocardial Revascularization, Recurrence, Risk Factors, Treatment Outcome, Coronary Thrombosis genetics, Gene Deletion, Peptidyl-Dipeptidase A genetics, Polymorphism, Genetic, Stents
Abstract

Background: The renin-angiotensin system is thought to play a role in coronary thrombosis and restenosis. Plasma angiotensin I-converting enzyme (ACE) activity is associated with an insertion/deletion polymorphism in the gene coding for ACE. The objective of this study was to test the hypothesis that the D allele of the ACE gene is associated with a higher risk for restenosis after coronary stent placement., Methods and Results: This prospective study included 1850 consecutive patients with coronary artery disease who underwent intracoronary stent implantation. The adverse clinical events recorded were death, myocardial infarction, and target vessel revascularization. The primary end point of the study was restenosis (>/=50% diameter stenosis at follow-up angiography performed in 84% of the patients). The secondary end point was clinical outcome 1 year after the procedure. The restenosis rate at the 6-month angiographic follow-up was 32.8% in patients with the II genotype, 34.0% for patients with the ID genotype, and 31.2% for patients with the DD genotype (P=0.62). One-year event-free survival was 77.7% in patients with genotype II, 75.2% in patients with genotype ID, and 75.5% in patients with genotype DD (P=0.54). The lack of association was also present in the subgroup of patients with a low risk for restenosis: the restenosis rate was 21.7% in II carriers, 23.4% in ID carriers, and 19.7% in DD carriers (P=0.83)., Conclusions: The ACE DD genotype or D allele does not influence the 1-year clinical and angiographic outcome of patients undergoing coronary stent placement. These data suggest that routine determination of the ACE genotype may not help identify patients who are at a higher risk of thrombotic and restenotic events after coronary stent placement.

Published
2000
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25. PlA polymorphism of glycoprotein IIIa and risk of adverse events after coronary stent placement.

Author

Kastrati A, Koch W, Gawaz M, Mehilli J, Böttiger C, Schömig K, von Beckerath N, and Schömig A

Subjects
Aged, Alleles, Angina Pectoris surgery, Antigens, CD metabolism, Antigens, Human Platelet blood, Coronary Angiography, Coronary Thrombosis blood, Coronary Thrombosis complications, Coronary Thrombosis diagnostic imaging, DNA analysis, DNA Primers chemistry, Epitopes blood, Epitopes genetics, Female, Genetic Markers, Genotype, Humans, Integrin beta3, Integrins blood, Integrins genetics, Male, Middle Aged, Myocardial Infarction blood, Myocardial Infarction diagnostic imaging, Myocardial Infarction etiology, Odds Ratio, Platelet Membrane Glycoproteins metabolism, Polymerase Chain Reaction, Prognosis, Prospective Studies, Risk Factors, Antigens, CD genetics, Antigens, Human Platelet genetics, Coronary Thrombosis genetics, Platelet Membrane Glycoproteins genetics, Polymorphism, Genetic, Stents adverse effects
Abstract

Objective: We designed this prospective study to test the hypothesis that platelet antigen (PlA) polymorphism of glycoprotein (GP) IIIa is associated with an increased risk for adverse events after coronary stent placement., Background: Platelets play a central role in arterial thrombosis. The PlA polymorphism of GP IIIa, a constituent of the fibrinogen receptor, may influence the platelet function and, thereby, the early outcome of patients after coronary stent placement., Methods: The study included 1,759 consecutive patients with stable or unstable angina and successful coronary stent placement. Platelet antigen genotypes were determined by allele-specific restriction enzyme analysis. The end point of the study was a composite of death, myocardial infarction and urgent revascularization during the first 30 days after stent placement., Results: The PlA1 genotype of the patients included was: 70.2% were homozygous for platelet antigen 1 (PlA1), 2.6% homozygous for platelet antigen 2 (PlA1), and 27.2% were heterozygous (PlA1/A2). The incidence of the composite end point was 5.5% among PlA2 carriers and 5.4% in homozygous PlA1 subjects (p = 0.94). It was 5.4% in PlA1/A1 patients, 4.8% in PlA1/A2 patients and 13.0% in PlA2A2 patients (p = 0.06). The combined incidence of death or myocardial infarction was 4.3% in PlA1/A1 patients, 4.2% in PlA1/A2 patients and 13.0% in PlA2/A2 patients (p = 0.02)., Conclusions: The isolated presence of the PlA2 allele in heterozygous patients is not associated with any detectable increase in the risk for an adverse 30-day outcome after coronary stenting. This study suggests also that an increased risk is likely to be present in homozygous carriers of the PlA2 allele, but this should be confirmed in a much larger series of patients.

Published
2000
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26. Glycoprotein Ia gene C807T polymorphism and risk for major adverse cardiac events within the first 30 days after coronary artery stenting.

Author

von Beckerath N, Koch W, Mehilli J, Böttiger C, Schömig A, and Kastrati A

Subjects
Aged, Amino Acid Substitution, Angina Pectoris diagnostic imaging, Angina Pectoris therapy, Angina, Unstable diagnostic imaging, Angina, Unstable therapy, Coronary Angiography, Coronary Disease diagnostic imaging, Coronary Disease mortality, DNA blood, Female, Genotype, Humans, Integrin beta1 physiology, Male, Middle Aged, Polymerase Chain Reaction, Receptors, Collagen, Recurrence, Risk Factors, Coronary Disease therapy, Integrins genetics, Polymorphism, Genetic, Stents adverse effects
Abstract

The glycoprotein complex Ia/IIa (GP Ia/IIa) is a major collagen receptor on platelets and other cell types. Recently, linked polymorphisms within the coding region of the GP Ia gene (C807T and G873A) were identified that are related to GP Ia/IIa surface expression. The T807/A873 allele is associated with high expression, whereas the C807/G873 allele is associated with low surface expression of GP Ia/IIa. Subsequently, the T807 allele was found to be associated with coronary and cerebral infarction in younger patients. Platelet adhesion to the vessel wall plays a pivotal role in thrombosis after coronary artery stent placement. The goal of this study was to test whether C807T polymorphism is associated with a higher incidence of thrombotic events following coronary stenting. Consecutive patients treated with coronary stent placement (n = 1797) were genotyped for C807T polymorphism with polymerase chain reaction and allele-specific fluorogenic probes. The composite end point was defined as death, myocardial infarction, or urgent target vessel revascularization within 30 days of stent implantation. The genotype distribution of the study population was CC in 36.5%, CT in 46.7%, and TT in 16.8% of the patients. The incidence of the composite end point was 6.5% in T allele carriers and 5.3% in noncarriers (odds ratio for T allele carriage 1.23 [95% confidence interval, 0.81-1.86], P =.33). After adjusting for other baseline characteristics, the odds ratio for the composite end point was 1.15 (0.76-1.75). Therefore, C807T genotype has no significant influence on the major adverse events occurring after coronary artery stenting.

Published
2000

27. HPA-1 and HPA-3 polymorphisms of the platelet fibrinogen receptor and coronary artery disease and myocardial infarction.

Author

Böttiger C, Kastrati A, Koch W, Mehilli J, Seidl H, Schömig K, von Beckerath N, and Schömig A

Subjects
Aged, Blood Donors, Coronary Angiography, Coronary Disease diagnostic imaging, Female, Gene Frequency, Genetic Predisposition to Disease, Genotype, Humans, Integrin beta3, Male, Middle Aged, Myocardial Infarction diagnostic imaging, Risk Factors, Antigens, Human Platelet genetics, Coronary Disease genetics, Myocardial Infarction genetics, Platelet Glycoprotein GPIIb-IIIa Complex genetics, Polymorphism, Genetic
Abstract

Platelet fibrinogen receptor (glycoprotein [GP] IIb/IIIa) plays a fundamental role in atherothrombosis. The human platelet antigen (HPA) -1 and the HPA-3 are the most extensively studied polymorphisms of GPIIIa and GPIIb, respectively. This study was designed to test, in a large population, the hypothesis that these polymorphisms represent a risk factor for the occurrence of coronary artery disease (CAD) and myocardial infarction (MI). Consecutive, angiographically examined patients with significant coronary stenoses but without symptoms or signs of old or acute MI constituted the group with CAD (CAD, n = 998) and those with old or acute MI constituted the group with MI (MI, n = 793). As controls served subjects, matched with patients for age and sex, with neither angiographic CAD nor symptoms or signs of MI (matched controls [MC], n = 340) as well as a group of blood donors without cardiac symptoms or signs of CAD (BD, n = 104). Genotype distribution was similar across the groups; HPA-1a/a: HPA-1a/b: HPA-1b/b was 75.0%: 22.1%: 2.9% in BD, 72.6%: 24.7%: 2.6% in MC, 70.5%: 26.8%: 2.7% in CAD, and 70.7%: 26.4%: 2.9% in MI; HPA-3a/a: HPA-3a/b: HPA-3b/b was 39.4%: 40.4%: 20.2% in BD, 33.5%: 50.0%: 16.5% in MC, 35.0%: 46.4%: 17.0% in CAD, and 37.1%: 48.0%: 16.5% in MI. There was no interaction between these polymorphisms, nor between each of these polymorphisms and other risk factors. Thus, the HPA-1 and HPA-3 polymorphisms are neither separately nor in concert associated with any measurable increase of the risk for CAD or MI in angiographically evaluated subjects.

Published
2000

28. G protein beta3 subunit polymorphism and risk of thrombosis and restenosis following coronary stent placement.

Author

von Beckerath N, Kastrati A, Koch W, Böttiger C, Mehilli J, Seyfarth M, and Schömig A

Subjects
Aged, Base Sequence, Coronary Angiography, Coronary Artery Bypass methods, Coronary Disease diagnostic imaging, Coronary Thrombosis epidemiology, Female, Follow-Up Studies, GTP-Binding Proteins analysis, Genotype, Graft Occlusion, Vascular epidemiology, Humans, Incidence, Logistic Models, Male, Middle Aged, Molecular Sequence Data, Multivariate Analysis, Polymerase Chain Reaction, Polymorphism, Genetic, Risk Factors, Stents adverse effects, Coronary Artery Bypass adverse effects, Coronary Disease genetics, Coronary Disease surgery, Coronary Thrombosis genetics, GTP-Binding Proteins genetics, Graft Occlusion, Vascular genetics
Abstract

C825T polymorphism in the G protein beta3 subunit gene (GNB3) has been associated with arterial hypertension, coronary artery disease and myocardial infarction. On the cellular level, C825T polymorphism is associated with altered transmembrane signaling via adenylyl cyclase inhibiting (G(i)) G proteins. This study was designed to test whether C825T polymorphism has an impact on the processes leading to restenosis and thrombosis following coronary stenting. The primary endpoint of the study was angiographic restenosis (> or =50% diameter stenosis) at 6-month follow-up. Secondary endpoint was angiographically proven stent thrombosis within 30 days of implantation. In the 562 consecutive patients C825T genotype was CC, 46.1%, CT, 45.2% and TT, 8.7%. The incidence of angiographic restenosis was 32.7% in homozygous carriers of the C allele, 28.2% in CT patients and 33.3% in homozygous carriers of the T allele (P = 0.563). C825T genotype distribution in 34 consecutive patients with subacute stent thrombosis (44.0% CC, 50.0% CT, and 6.0% TT) was not different from that of 451 patients with angiographically patent stented vessel (45.4% CC, 44.6% CT, 10.0% TT; P = 0.644). In conclusion, C825T polymorphism has no appreciable impact on the mechanisms leading to thrombosis and restenosis following coronary stent placement.

Published
2000
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29. Polymorphism of platelet glycoprotein IIb and risk of thrombosis and restenosis after coronary stent placement.

Author

Böttiger C, Kastrati A, Koch W, Mehilli J, von Beckerath N, Dirschinger J, Gawaz M, and Schömig A

Subjects
Adult, Aged, Coronary Angiography, Coronary Disease therapy, Coronary Thrombosis therapy, Female, Follow-Up Studies, Gene Frequency, Genetic Predisposition to Disease genetics, Genotype, Humans, Male, Middle Aged, Prospective Studies, Recurrence, Treatment Outcome, Angioplasty, Balloon, Coronary instrumentation, Coronary Disease genetics, Coronary Thrombosis genetics, Platelet Glycoprotein GPIIb-IIIa Complex genetics, Polymorphism, Genetic genetics, Stents
Abstract

Both glycoprotein (GP) IIb and IIIa of platelet fibrinogen receptor are polymorphic proteins. Unlike GPIIIa, there is little information about the clinical significance of the GPIIb polymorphism. We designed this prospective study to assess whether patients with the human platelet antigen (HPA)-3 polymorphism of GPIIb are more susceptible to developing thrombosis and restenosis after coronary stent placement. We included 2,178 consecutive patients with coronary artery disease who underwent intracoronary stent implantation, 789 (36.2%) with HPA-3a/a, 1,023 (47.0%) with HPA-3a/b, and 366 (16.8%) with HPA-3b/b genotype. The incidence of stent thrombosis was 1.7% in HPA-3a/a, 1.7% in HPA-3a/b, and 1.6% in HPA-3b/b patients (p = 0.999). The incidence of stent restenosis was 37.3% in HPA-3a/a, 36.2% in HPA-3a/b, and 34.6% in HPA-3b/b patients (p = 0.724). Event-free survival 1 year after stent placement was 76.1% for HPA-3a/a, 76.5% for HPA-3a/b, and 76.4% for HPA-3b/b patients (p = 0.968). We conclude that the HPA-3 polymorphism of platelet GPIIb is not associated with an increase in the risk of thrombosis and restenosis over 1 year after coronary stent placement. These data indicate that unlike the HPA-1 polymorphism of GPIIIa, the HPA-3 polymorphism of GPIIb may not serve as a useful genetic marker for the risk assessment of patients treated with intracoronary stenting.

Published
1999
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30. PlA polymorphism of platelet glycoprotein IIIa and risk of restenosis after coronary stent placement.

Author

Kastrati A, Schömig A, Seyfarth M, Koch W, Elezi S, Böttiger C, Mehilli J, Schömig K, and von Beckerath N

Subjects
Adult, Aged, Alleles, Coronary Disease etiology, Female, Genotype, Humans, Male, Middle Aged, Prospective Studies, Recurrence, Risk, Coronary Disease therapy, Platelet Glycoprotein GPIIb-IIIa Complex genetics, Polymorphism, Genetic, Stents
Abstract

Background: Platelets play a central role in the process of restenosis after percutaneous coronary interventions. A polymorphism of platelet glycoprotein IIIa (PlA) has been associated with a higher risk of coronary thrombosis. We designed this prospective study to test the hypothesis that PlA polymorphism of glycoprotein IIIa is associated with an increased risk for restenosis after coronary stent placement., Methods and Results: The study included 1150 consecutive patients with successful coronary stent placement and 6-month follow-up with coronary angiography. The end point of the study was the incidence of angiographic restenosis (>/=50% diameter stenosis) at follow-up. Of the 1150 patients, 72.5% were homozygous for PlA1, 24.7% were heterozygous (PlA1/A2), and 2.8% were homozygous for PlA2. Patients with the PlA2 allele demonstrated a significantly higher restenosis rate than did those without (47% versus 38%; OR, 1.42; 95% CI, 1.09 to 1.84). The risk was highest in homozygous carriers of PlA2 (53.1% restenosis rate). After adjustment for several clinical and angiographic characteristics, the presence of the PlA2 allele remained a significantly independent risk factor for restenosis (adjusted OR, 1.35; 95% CI, 1.07 to 1.70). The influence of the PlA2 allele on restenosis was stronger in women. Women with PlA2 had a restenosis rate of 52% compared with the 33% incidence among women homozygous for PlA1 (OR, 2.21; 95% CI, 1.27 to 3.85)., Conclusions: This study showed a significant association between the PlA polymorphism of glycoprotein IIIa and the risk of restenosis after coronary stent placement. The risk was more pronounced in patients homozygous for PlA2 allele and in female patients.

Published
1999
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