Intermittent claudication is a common problem which causes significant impairment of quality of life and increased mortality. Endovascular recanalization, widely used for symptomatic relief, carries a high risk of reocclusion. Platelets play a central role in this process. Aspirin currently used in claudicants reduces the risk, and more potent antiplatelet strategies may reduce this further. The aim of this study was to investigate the antiplatelet effect of aspirin–clopidogrel versus aspirin alone in patients with claudication undergoing endovascular intervention. Methods: This was a double-blind randomized placebo-controlled trial; 132 patients were randomized to clopidogrel and aspirin or to placebo and aspirin with a loading dose 12 h before endovascular intervention. Flow cytometric measurement of platelet fibrinogen binding and P-selectin expression as measures of platelet activation status and of platelet responsiveness to stimulation at baseline, 12 h post-loading dose, 1 h, 24 h and 30 days postintervention. Results: Platelet activation was significantly diminished in the clopidogrel group at 12 h post-loading dose compared to baseline (P-selectin: 27·3 per cent reduction, P = 0·017; bound fibrinogen: 34·7 per cent reduction, P = 0·024; stimulated bound fibrinogen: 49 per cent, P < 0·001). No significant change was observed in the control group. Platelet function was significantly suppressed in the clopidogrel group at 1 h, 24 h and 30 days after endovascular intervention compared to the placebo group (P < 0·001). Conclusion: Clopidogrel–aspirin combination dramatically inhibits platelet function in claudicants before and after intervention. The combination treatment may help reduce reocclusion after endovascular recanalization.peer-reviewe

Bachoo, Paul

Brittenden, Julie

Cassar, Kevin

Ford, Isobel

Greaves, Mike

OAR@UM

1214 SARS abstractsDecreased skeletal muscle necrosis and remote lung injury in c-JunN-terminal kinase 2 knockout mice after lower-limbischaemia–reperfusion injuryD. W. Harkin, N. Degousee, E. Stefanski, T. F. Lindsay, M. Karin andB. B. RubinDivision of Vascular Surgery, Department of Surgery, The Toronto Hospital (GeneralDivision), Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada andRegional Vascular Surgery Unit, Royal Victoria Hospital Belfast, Belfast, UKBackground: Skeletal muscle ischaemia–reperfusion (I-R) injury initiatesan inflammatory response characterized by neutrophil activation and remoteacute lung injury. The purpose of this study was to define the role of c-Jun N-terminal kinase (JNK) enzymes, implicated in the regulation of the inflammatoryresponse, in skeletal muscle and lung injury following lower-limb I-R.Methods: JNK1- and JNK2-knockout (ko) mice or their wild-type (wt)littermates were subjected to 180 min of unilateral hindlimb tourniquetischaemia, followed by 24 h reperfusion. Gastrocnemius muscle viability wasmeasured by nitroblue tetrazolium staining and computerized planimetry.Myeloperoxidase (MPO) and wet weight measured neutrophil sequestrationand oedema respectively.Results: Skeletal muscle viability following lower-extremity I-R wassignificantly increased in JNK2-ko mice compared to JNK2-wt controls(52·8(6·9) versus 0·2(0·1) per cent; P < 0·004). Skeletal muscle oedema wassignificantly reduced in JNK2-ko mice compared to JNK2-wt controls (1·2(0·1)versus 1·6(0·1); P < 0·04). Skeletal muscle MPO was significantly increased inJNK2-ko mice compared to JNK2-wt controls (0·019(0·004) versus 0·007(0·004);P < 0·02). Lung tissue MPO was significantly reduced in JNK2-ko micecompared to JNK2-wt controls (0·049(0·009) versus 0·195(0·06); P < 0·01).JNK1-ko mice resembled controls. Values are mean(s.e.m.); ANOVA andScheffé’s test.Conclusion: This is the first study to evaluate the role of a JNK isoforms inskeletal muscle injury, and clearly shows that JNK2 participates in the sequenceof events that culminates in muscle necrosis and remote acute lung injury.Inhibition of JNK2 activity may decrease muscle necrosis in those patientswith limb ischaemia, and protect against acute neutrophil-mediated pulmonarydamage.Type 1 tyrosine kinase receptor coexpression is a predictor ofrecurrence in ductal carcinoma in situ (DCIS) of the breastN. L. P. Barnes, G. P. Boland, S. Khavari, A. Cramer, W. F. Knox andN. J. BundredSouth Manchester University Hospital and The Paterson Institute for Cancer Research,Manchester, UKBackground: Human epidermal growth factor receptor (HER) 2 overex-pression is associated with endocrine resistance and early recurrence in invasivebreast tumours. Expression of HER2, and other type 1 tyrosine kinase receptors,may predict risk of recurrence after surgery for DCIS; recurrences occur in upto 20 per cent of patients at 5 years, after breast-conserving surgery and radio-therapy. To determine if HER2 and HER4 expression predicted recurrence ofDCIS we studied the primary DCIS of 133 women (follow-up 3–12 years), 94who had not recurred and 39 who had recurred (27 with recurrent DCIS, 12with invasive disease).Methods: Tumours were compared for HER2, HER4 and oestrogen receptor(ER) expression by immunohistochemistry. HER2/4 expression was scored 0(absent) to 3 (maximum). Scores ≥ 2 were taken as overexpression. ER wasscored positive if ≥ 5 per cent of cells stained.Results: Of non-recurrent DCIS lesions, 57 per cent were HER2 positiveand 64 per cent HER4 positive, compared to 82 per cent HER2 positive(P = 0·007*) and 36 per cent HER4 positive (P = 0·003*) in the recurrentgroup. HER2/HER4 coexpression was associated with reduced recurrencecompared to HER2-positive tumours lacking HER4 (P = 0·003*). Thisassociation remained significant when stratifying for high grade (P = 0·015*)and breast-conserving surgery (P < 0·001*). HER4-positive DCIS was morelikely to be ER positive than HER2-overexpressing DCIS (74 versus 51 per cent;P = 0·048*). ER status did not influence recurrence in HER4-positive tumours(P = 0·8*). *χ2 test.No recurrence(n = 94)Recurrence(n = 39)HER2neg/HER4neg 11 (12) 5 (130)HER2pos/HER4neg 23 (24) 20 (51)HER2neg/HER4pos 29 (31) 2 (5)HER2pos/HER4pos 31 (33) 12 (31)Values in parentheses are percentages. P = 0·003 (χ2 test).Conclusion: Overexpression of HER2 in the absence of HER4 increases riskof early recurrence of DCIS.Colorectal cancers with microsatellite instability demonstrate mRNAexpression signatures characteristic of increased immunogenicityA. Banerjea, S. Ahmed, R. Hands, F. Huang, P. M. Shaw, S. A. Bustinand S. DorudiCentre for Academic Surgery, The Royal London Hospital, Barts and The LondonQueen Mary School of Medicine and Dentistry, London, UK and Department ofPharmacogenomics, Bristol-Myers Squibb, New Jersey, USABackground: Colorectal cancers with high-degree microsatellite instability(MSI-H) have an improved prognosis compared to microsatellite stable (MSS)cancers. The observation of pronounced lymphocytic infiltrates suggests thatMSI-H cancers are inherently more immunogenic.Methods: We analysed tissue from 133 colorectal cancers with full consent andlocal ethics committee approval. Genomic DNA was analysed for microsatelliteinstability in BAT-26. High-quality RNA was used for microarray analysison the Affymetrix HG-U133A chip (using Affymetrix protocols). Data wereanalysed on GeneSpring software version 6.0. Confirmatory real-time reversetranscriptase–polymerase chain reaction (RT-PCR) was performed on 28 MSI-H and 26 MSS cancers.Results: Twenty-nine colorectal cancers (22 per cent) were identified as MSI-H. A comparison with 104 MSS cancers identified 2070 genes that weredifferentially expressed between the two groups (P < 0·005, Benjamini andHochberg False Discovery Rate). Significantly, several key immunomodulatorygenes were upregulated in MSI-H cancers. These included antigen chaperonemolecules (heat shock protein (HSP) 70, HSP-110, calreticulin, gp96),proinflammatory cytokines (interleukin (IL) 18, IL-8, IL-15, IL-24, IL-7)and cytotoxic mediators (granulysin, granzyme A). Quantitative RT-PCRconfirmed upregulation of HSP-70(1b) (P = 0·016), HSP-110 (P = 0·002),IL-18 (P = 0·004), IL-8 (P = 0·002) and granulysin (P < 0·001).Conclusion: The novel observation of HSP upregulation in MSI-H colorectalcancer is highly significant in light of the recognized role of these proteinsin innate and antigen-specific immunogenicity. Increased mRNA levels ofproinflammatory cytokines and cytotoxic mediators also indicate an activatedantitumour response. MSI-H colorectal cancer may be a paradigm of aninherent antigen-specific immune response and its study may significantlyadvance our understanding of tumour immunology and the development ofimmunotherapeutic strategies.Double-blind randomized placebo-controlled trial of the antiplateleteffects of aspirin–clopidogrel combination versus aspirin alone atendovascular intervention for intermittent claudication of the lowerlimbK. Cassar, P. Bachoo, I. Ford, M. Greaves and J. BrittendenDepartments of Vascular Surgery, and Medicine and Therapeutics, University ofAberdeen and Vascular Unit, Aberdeen Royal Infirmary, Aberdeen, UKBackground: Intermittent claudication is a common problem which causessignificant impairment of quality of life and increased mortality. Endovascularrecanalization, widely used for symptomatic relief, carries a high risk ofreocclusion. Platelets play a central role in this process. Aspirin currentlyused in claudicants reduces the risk, and more potent antiplatelet strategies mayCopyright  2004 British Journal of Surgery Society Ltd www.bjs.co.uk British Journal of Surgery 2004; 91: 1206–1238Published by John Wiley & Sons LtdDownloaded from https://academic.oup.com/bjs/article/91/9/1213/6143778 by University of Malta user on 29 July 2022SARS abstracts 1215reduce this further. The aim of this study was to investigate the antiplateleteffect of aspirin–clopidogrel versus aspirin alone in patients with claudicationundergoing endovascular intervention.Methods: This was a double-blind randomized placebo-controlled trial; 132patients were randomized to clopidogrel and aspirin or to placebo and aspirinwith a loading dose 12 h before endovascular intervention. Flow cytometricmeasurement of platelet fibrinogen binding and P-selectin expression asmeasures of platelet activation status and of platelet responsiveness to stimulationat baseline, 12 h post-loading dose, 1 h, 24 h and 30 days postintervention.Results: Platelet activation was significantly diminished in the clopidogrelgroup at 12 h post-loading dose compared to baseline (P-selectin: 27·3 per centreduction, P = 0·017; bound fibrinogen: 34·7 per cent reduction, P = 0·024;stimulated bound fibrinogen: 49 per cent, P < 0·001). No significant changewas observed in the control group. Platelet function was significantly suppressedin the clopidogrel group at 1 h, 24 h and 30 days after endovascular interventioncompared to the placebo group (P < 0·001).Conclusion: Clopidogrel–aspirin combination dramatically inhibits plateletfunction in claudicants before and after intervention. The combinationtreatment may help reduce reocclusion after endovascular recanalization.Co-activator and oestrogen receptor expression may determinetamoxifen resistance in breast cancerF. J. Fleming, A. D. K. Hill, E. W. McDermott, N. O’Higgins andL. S. YoungDepartment of Surgery and Conway Institute of Biomolecular and Biomedical Research,University College Dublin, IrelandIntroduction: The precise mechanism of tamoxifen resistance remains unclear.We examined the role of oestrogen receptor (ER) isoform expression and theco-activator proteins SRC-1and AIB-1 in tamoxifen resistance.Methods: The expression of ER-α, ER-β, AIB-1 and SRC-1 was evaluated inbreast cancer specimens by immunohistochemistry (n = 52).The ability of β-oestradiol and 4-hydroxytamoxifen (4-OHT) to modulate ER and co-regulatoryprotein expression in primary breast cancer cell cultures (n = 48) was assessedby western blotting. ER interaction with the oestrogen response element (ERE)in the presence of β-oestradiol and 4-OHT was assessed by electromobilityshift assays. ER-α/ER-β–co-regulatory protein interactions were assessed byimmunoprecipitation.Results:No. of patients(n = 52)Recurrence(n = 14)No recurrence(n = 38)ER-α positivity 40 (77) 10 (71) 30 (79)ER-β positivity 28 (54) 4 (29)* 24 (63)SRC-1 positivity 14 (26) 12 (84)† 2 (5)AIB-1 positivity 30 (57) 12 (84)‡ 18 (47)Values in parentheses are percentages. *P = 0·026, †P < 0·001,‡P = 0·01 versus no recurrence (χ2 test).β-Oestradiol upregulated ER-β and SRC-1 but not AIB-1 expression inimmunoblotting experiments and increased ER-α/ER-β interaction with theERE. 4-OHT increased ER-α and AIB-1 expression and increased AIB-1–EREbinding. ER-α and ER-β preferentially bound SRC-1 in the presence ofβ-oestradiol. 4-OHT potentiated ER-α–AIB-1 interaction while converselyinhibiting that of ER-β and AIB-1.Conclusion: The ability of ER-α, but not ER-β to recruit the co-activatorAIB-1 to the ER–ERE supports our clinical observation of ER-β as a positiveprognostic indicator. AIB-1 may therefore be an attractive therapeutic targetfor endocrine-resistant tumours.Patey Prize 2Matrix metalloproteinase l and 12 transcript levels correlate withhistopathological characteristics and clinical manifestations ofcarotid atherosclerotic plaquesN. Dastur, A. R. Morgan, K. Rerkasem, P. Gallagher, G. E. Morris,P. Eriksson, W. L. McPheat, C. P. Shearman and S. YeDepartment of Vascular Surgery and Human Genetics Division, Southampton GeneralHospital, Southampton, UKBackground: Previous studies have shown that atherosclerotic lesions expressa number of matrix metalloproteinases (MMPs) and that increased levels areassociated with histologically defined unstable plaques. We investigated whethertranscript levels of MMP-l, -3, -7, -9 and -12 in carotid atherosclerotic plaquescorrelated with histological features and clinical events.Methods: Atherosclerotic plaques (n = 50) removed from patients undergoingcarotid endarterectomy were classified histologically using a system proposedby Virmani et al., and MMP-l, -3, -7, -9 and -12 transcript levels in these tissuesquantified by real-time reverse transcriptase–polymerase chain reaction.Results: Comparing more stable plaques (with thick fibrous caps) to those lessstable plaques (with thin caps) there was a 7·8-fold higher MMP-l transcript level(P = 0·006), and 1·5–2·1-fold higher level of MMP-3, -7 and -12. MMP-12transcript levels were significantly increased in ruptured plaques compared withlesions without cap disruption (P = 0·001). MMP-l and -12 transcript levelswere significantly higher in plaques from patients with amaurosis fugax than inthose from asymptomatic patients (P = 0·029 and P = 0·008 for MMP-l andMMP-12 respectively).Conclusion: These data support a role for MMP-l and -12 in determiningatherosclerotic plaque stability and this is associated with clinical findings. Wepostulate that pharmacological modulation of MMPs could have a beneficialeffect on clinical outcome.Gefitinib (‘Iressa’, ZD1839) has activity in patients with oestrogenreceptor (ER)-negative breast cancer and ER-positive breast cancerthat has acquired resistance to tamoxifen: results from a phase IIstudyE. Gutteridge, K. L. Cheung, R. Owers, M. Koehler, L. Hamilton,J. Gee, R. I. Nicholson and J. F. R. RobertsonCity Hospital, University of Nottingham, Nottingham, UK, AstraZeneca, Wilmington,Delaware, USA and Luton, UK, and Tenovus Centre for Cancer Research, Cardiff, UKBackground: Control of cell proliferation in acquired resistance may bethrough alternative signalling mechanisms such as the epidermal growth factorreceptor (EGFR) pathway. This trial investigated in patients with tamoxifen(TAM)-resistant tumours and ER-negative breast cancer, the efficacy andsafety of the oral epidermal growth factor receptor–tyrosine kinase inhibitor(EGFR-TKI) gefitinib (‘Iressa’, ZD1839) 500 mg/day.Methods and results: For 33 patients the median (range) age was 61(32–85) years. Metastases included local regional disease and distant metastases.At 6 months, using Union Internacional Contra la Cancrum (UICC) criteria,gefitinib showed antitumour activity in both groups. Of the ER-positive patients(n = 9), one patient had a partial response (PR) and five had stable disease (SD).Of the ER-negative patients (n = 18), one had a PR, one had SD and 16patients had progressive disease. Gefitinib was generally well tolerated, withgenerally mild (grade 1 or 2) side-effects. Biopsies were assessed for EGFR,c-erbB2 and activated c-erbB2 using HScore analysis. In ER-positive tumours(n = 2), EGFR, c-erbB2 and activated c-erbB2 were coexpressed. This agreesCopyright  2004 British Journal of Surgery Society Ltd www.bjs.co.uk British Journal of Surgery 2004; 91: 1206–1238Published by John Wiley & Sons LtdDownloaded from https://academic.oup.com/bjs/article/91/9/1213/6143778 by University of Malta user on 29 July 2022European Colorectal Congress28 November – 1 December 2022, St.Gallen, SwitzerlandEUROPEAN  COLORECTAL  CONGRESS 202228 Nov – 1 Dec · St.Gallen · SwitzerlandInformation & Registration www.colorectalsurgery.euTuesday, 29 November 20229.00CONSULTANT‘S CORNERMichel Adamina, Winterthur, CH10.30COFFEE BREAK11.00SATELLITE SYMPOSIUM11.45Trends in colorectal oncology andclinical insights for the near futureRob Glynne-Jones, London, UK12.15LUNCH13.45VIDEO SESSION14.15SATELLITE SYMPOSIUM 15.00COFFEE BREAK15.30The unsolved issue of TME:open, robotic, transanal, or laparoscopic – shining light on evidence and practiceDes Winter, Dublin, IEJim Khan, London, UKBrendan Moran, Basingstoke, UK16.30SATELLITE SYMPOSIUM17.15Lars Pahlman lectureSøren Laurberg, Aarhus, DKWednesday, 30 November 2022 9.00 Advanced risk stratification in colorectal cancer – choosing wisely surgery and adjuvant therapyPhilip Quirke, Leeds, UK09.30Predictors for Postoperative Complications and MortalityRonan O‘Connell, Dublin, IE10.00Segmental colectomy versus extended colectomy for complex cancerQuentin Denost, Bordeaux, FR10.30COFFEE BREAK11.00Incidental cancer in polyp - completion surgery or endoscopy treatment alone?Laura Beyer-Berjot, Marseille, FR11.30SATELLITE SYMPOSIUM12.00Less is more – pushing the boundaries of full-thickness rectal resectionXavier Serra-Aracil, Barcelona, ES12.30LUNCH14.00Management of intestinal neuroendocrine neoplasiaFrédéric Ris, Geneva, CH 14.30Poster Presentation & Best Poster AwardMichel Adamina, Winterthur, CH15.00SATELLITE SYMPOSIUM15.45COFFEE BREAK16.15Reoperative pelvic floor surgery – dealing with perineal hernia, reoperations, and complex reconstructionsGuillaume Meurette, Nantes, FR16.45Salvage strategies for rectal neoplasiaRoel Hompes, Amsterdam, NL17.15Beyond TME – technique and results of pelvic exenteration and sacrectomyParis Tekkis, London, UK19.30FESTIVE EVENINGMonday, 28 November 202209.50Opening and welcomeJochen Lange, St.Gallen, CH10.00It is leaking! Approaches to salvaging an anastomosisWillem Bemelman, Amsterdam, NL10.30Predictive and diagnostic markersof anastomotic leakAndre D‘Hoore, Leuven, BE11.00SATELLITE SYMPOSIUM11.45Of microbes and men – the unspoken story of anastomotic leakageJames Kinross, London, UK12.15LUNCH13.45Operative techniques to reduce anastomotic recurrence in Crohn’s diseaseLaura Hancock, Manchester, UK14.15Innovative approaches in the treatment of complex Crohn Diseases perianal fistulaChristianne Buskens, Amsterdam, NL14.45To divert or not to divert in Crohn surgery – technical aspects and patient factorsPär Myrelid, Linköping, SE15.15COFFEE BREAK15.45Appendiceal neoplasia – when to opt for a minimal approach, when and how to go for a maximal treatmentTom Cecil, Basingstoke, Hampshire, UK16.15SATELLITE SYMPOSIUM17.00Outcomes of modern induction therapies and Wait and Watch strategies, Hope or HypeAntonino Spinelli, Milano, IT17.30EAES Presidential Lecture - Use of ICG in colorectal surgery: beyond bowel perfusionSalvador Morales-Conde, Sevilla, ES18.00Get-Together with your colleaguesIndustrial ExhibitionThursday, 1 December 2022Masterclass in Colorectal SurgeryProctology Day

Double-blind randomized placebo-controlled trial of the antiplatelet effects of aspirin-clopidogrel combination versus aspirin alone at endovascular intervention for intermittent claudication of the lower limb

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Double-blind randomized placebo-controlled trial of the antiplatelet effects of aspirin-clopidogrel combination versus aspirin alone at endovascular intervention for intermittent claudication of the lower limb

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