Book contents
- Frontmatter
- Contents
- Contributors
- Preface
- Foreword
- Abbreviations
- SECTION 1 Admission to Critical Care
- SECTION 2 General Considerations in Cardiothoracic Critical Care
- SECTION 3 System Management in Cardiothoracic Critical Care
- 3.1 CARDIOVASCULAR SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 19 Rhythms
- 20 Basic haemodynamic support
- 21 Mechanical circulatory support
- 22 Systemic hypertension
- 23 Pulmonary hypertension
- 3.2 RESPIRATORY SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 3.3 RENAL SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 3.4 HAEMATOLGY AND TRANSFUSION IN CARDIOTHORACIC CRITICAL CARE
- 3.5 GASTROINTESTINAL SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 3.6 IMMUNE SYSTEM AND INFECTION IN CARDIOTHORACIC CRITICAL CARE
- 3.7 ENDOCRINE SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 3.8 NEUROLOGICAL SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- SECTION 4 Procedure-Specific Care in Cardiothoracic Critical Care
- SECTION 5 Discharge and Follow-up From Cardiothoracic Critical Care
- SECTION 6 Structure and Organisation in Cardiothoracic Critical Care
- SECTION 7 Ethics, Legal Issues and Research in Cardiothoracic Critical Care
- Appendix Works Cited
- Index
20 - Basic haemodynamic support
from 3.1 - CARDIOVASCULAR SYSTEM IN CARDIOTHORACIC CRITICAL CARE
Published online by Cambridge University Press: 05 July 2014
- Frontmatter
- Contents
- Contributors
- Preface
- Foreword
- Abbreviations
- SECTION 1 Admission to Critical Care
- SECTION 2 General Considerations in Cardiothoracic Critical Care
- SECTION 3 System Management in Cardiothoracic Critical Care
- 3.1 CARDIOVASCULAR SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 19 Rhythms
- 20 Basic haemodynamic support
- 21 Mechanical circulatory support
- 22 Systemic hypertension
- 23 Pulmonary hypertension
- 3.2 RESPIRATORY SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 3.3 RENAL SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 3.4 HAEMATOLGY AND TRANSFUSION IN CARDIOTHORACIC CRITICAL CARE
- 3.5 GASTROINTESTINAL SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 3.6 IMMUNE SYSTEM AND INFECTION IN CARDIOTHORACIC CRITICAL CARE
- 3.7 ENDOCRINE SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- 3.8 NEUROLOGICAL SYSTEM IN CARDIOTHORACIC CRITICAL CARE
- SECTION 4 Procedure-Specific Care in Cardiothoracic Critical Care
- SECTION 5 Discharge and Follow-up From Cardiothoracic Critical Care
- SECTION 6 Structure and Organisation in Cardiothoracic Critical Care
- SECTION 7 Ethics, Legal Issues and Research in Cardiothoracic Critical Care
- Appendix Works Cited
- Index
Summary
Introduction
Cardiac surgical patients often present for surgery with impaired ventricular contractility owing to chronic ischaemia or valve lesions. The heart is then subjected to a surgical procedure, which produces a period of global ischaemia and a massive, whole-body inflammatory response. The deleterious effects of cardiopulmonary bypass (CPB) are due to activation of the coagulation, fibrinolytic and complement pathways. This may lead to postoperative adverse effects, including extravascular fluid accumulation or ‘third spacing,’ coagulopathy and haemorrhage, and pulmonary, renal, cardiac and vasomotor dysfunction.
The perioperative period is often a time of significant haemodynamic and vasomotor instability. Ventricular contractility is usually impaired for up to 24 hours, which may respond to simple supportive measures such as fluid administration. When more severe, there may be a reduction in blood pressure and cardiac output (CO) associated with end-organ dysfunction. Under these circumstances, haemodynamic support is required.
Optimize the heart rate
The CO is a product of stroke volume (SV) and heart rate (HR). Generally, a postoperative HR of 80 to 100 beats per minute is regarded as optimal. The most frequent postoperative rhythm problem is bradycardia. This may be related to preoperative β-blockade or postoperative nodal dysfunction.
Increasing the HR in bradycardic patients improves CO. In addition, by decreasing diastolic filling time and reducing the end-diastolic volume (EDV), left ventricular (LV) wall tension is reduced and the perfusion of the subendocardium is improved, reducing the potential for ischaemia.
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- Information
- Core Topics in Cardiothoracic Critical Care , pp. 146 - 156Publisher: Cambridge University PressPrint publication year: 2008