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Circulatory system

The circulatory system, also known as the cardiovascular system, is an organ system that includes the heart, blood vessels, and blood, functioning to transport oxygen, nutrients, hormones, and cellular waste products throughout the body while removing carbon dioxide and other metabolic byproducts. It ensures the delivery of essential substances to cells and maintains homeostasis by regulating interstitial fluid composition and supporting tissue oxygenation via bulk flow of blood through capillaries. The heart serves as the central pump of the system, a muscular organ approximately the size of a fist, divided into four chambers: two atria that receive blood and two ventricles that pump it out. Blood flows through a closed network of vessels, including elastic arteries that carry oxygenated blood away from the heart under high pressure, thin-walled capillaries where exchange of gases and nutrients occurs, and veins equipped with valves that return deoxygenated blood to the heart. The system operates in two interconnected loops: the pulmonary circulation, where the right ventricle pumps blood to the lungs for oxygenation and carbon dioxide removal, and the systemic circulation, where the left ventricle propels oxygenated blood to the body's tissues via the aorta and its branches. Key physiological functions are regulated by factors such as —calculated as multiplied by —to match venous return and maintain adequate . , which decreases progressively from arteries to veins due to , is controlled by the , hormones, and local autoregulatory mechanisms like myogenic responses in arterioles and metabolic signals such as . This dynamic regulation ensures that oxygen delivery adapts to metabolic demands, with in red blood cells facilitating transport and releasing signaling molecules like ATP to promote during . Overall, the circulatory system's efficiency is vital for , as every must remain within about 10 micrometers of a for effective diffusion-based exchange.

Structure

Heart

The heart is a muscular organ about the size of a closed fist, weighing approximately 250–350 grams in adults, located in the within the . It is enclosed by the , a double-layered sac consisting of an outer fibrous pericardium that anchors the heart and an inner serous pericardium (parietal and visceral layers) that reduces friction during contractions. The heart wall comprises three layers: the outer epicardium (visceral pericardium, a thin layer of and fat), the thick middle myocardium composed of cells (cardiomyocytes) arranged in a helical pattern for efficient pumping, and the inner , a thin endothelium-lined layer continuous with blood vessels that lines the chambers and valves. Internally, the heart is divided into four chambers: the right and left atria (upper chambers that receive ) and the right and left ventricles (lower chambers that pump ). The atria are separated by the , and the ventricles by the , which includes a thick muscular portion and a thinner membranous part. The right ventricle pumps to the lungs, while the left ventricle, with thicker walls (about 1–1.5 cm vs. 0.3–0.5 cm for the right), propels to the systemic circulation. Four valves ensure unidirectional blood flow: the (between right atrium and ventricle) and mitral (bicuspid) valve (between left atrium and ventricle) are atrioventricular valves with fibrous rings, attaching cusps to papillary muscles, and three (tricuspid) or two (mitral) cusps. The semilunar valves include the (right ventricle to pulmonary trunk) and (left ventricle to ), each with three crescent-shaped cusps that prevent backflow during .

Blood

Blood is a specialized fluid connective tissue that serves as the primary transport medium in the circulatory system, consisting of and formed elements suspended within it. It circulates continuously, delivering essential substances while removing waste, with its composition optimized for fluidity and function.

Plasma

Plasma constitutes approximately 55% of total and is a straw-colored composed mainly of (about 90-92%), which acts as the for various solutes. The remaining 8-10% includes proteins such as (3.5-5.0 g/dL, responsible for maintaining colloidal ), globulins (including immunoglobulins for immune defense), and fibrinogen (involved in clotting). Electrolytes like sodium, potassium, chloride, and maintain osmotic balance and ; nutrients such as glucose and support cellular ; hormones regulate physiological processes; and waste products like and are transported for .

Formed Elements

The formed elements make up the remaining 45% of blood and include erythrocytes, leukocytes, and thrombocytes, all primarily produced in the bone marrow. Erythrocytes, or red blood cells, are biconcave discs lacking a nucleus, numbering about 4.5-6.0 million per microliter in adults, and contain hemoglobin for oxygen transport. Hemoglobin is a tetrameric protein with four heme groups, each binding one oxygen molecule via a central ferrous iron atom, enabling reversible oxygen attachment in the lungs and release in tissues. Leukocytes, or , are nucleated cells averaging 4,000-11,000 per microliter, crucial for immune defense. Neutrophils (50-70% of leukocytes) phagocytose ; lymphocytes (20-40%), including B cells for production and T cells for cellular immunity, orchestrate adaptive responses; monocytes (2-8%) differentiate into macrophages for ; eosinophils (1-4%) combat parasites and modulate allergies; and basophils (<1%) release histamine in allergic reactions. Thrombocytes, or platelets, are small anucleate fragments (150,000-450,000 per microliter) derived from , essential for hemostasis by adhering to damaged vessel walls and aggregating to form a plug.

Blood Volume, Hematocrit, and Viscosity

In a typical adult, total blood volume is approximately 5 liters (about 70-75 mL/kg body weight), varying by sex, size, and hydration status, with women generally having lower volumes than men. Hematocrit, the percentage of blood volume occupied by , ranges from 36-48% in females and 40-54% in males, reflecting the proportion of cellular to plasma components. Blood viscosity, which influences flow resistance, is primarily determined by hematocrit (higher levels increase viscosity), plasma protein concentration, erythrocyte deformability, and aggregation tendencies, ensuring efficient circulation without excessive resistance.

Blood Groups

Human blood is classified into ABO groups based on carbohydrate antigens on erythrocyte surfaces: type A (A antigens), B (B antigens), AB (both), and O (neither), determined by alleles at the ABO locus. The Rh system adds the D antigen, classifying blood as Rh-positive (present) or Rh-negative (absent), critical for transfusion compatibility to prevent immune reactions.

Clotting Cascade

The clotting cascade is a series of enzymatic reactions culminating in hemostasis, where thrombin (factor IIa) cleaves fibrinogen into fibrin monomers that polymerize into a stable mesh, cross-linked by factor XIII to form the clot scaffold. This process, involving both intrinsic and extrinsic pathways converging on the common pathway, prevents excessive bleeding while platelets provide the initial plug.

Blood vessels

Blood vessels form a closed network that transports blood throughout the body, classified into , , and based on structure and function in circulation. Arteries carry blood away from the heart, typically oxygenated except for the . They have thick walls to withstand high pressure, consisting of three layers: the (inner endothelium and subendothelial connective tissue), (smooth muscle and elastic fibers for elasticity and contraction), and (outer connective tissue anchoring the vessel). Elastic arteries (e.g., ) have abundant elastic laminae for pulse propagation, while muscular arteries (e.g., ) have more smooth muscle for vasoregulation. Arterioles, smaller branches, further regulate flow via smooth muscle tone. Capillaries are the smallest vessels (5–10 μm diameter), sites of exchange between blood and tissues. They consist of a single layer of endothelial cells with a basement membrane, lacking tunica media and adventitia, allowing diffusion of gases, nutrients, and wastes. Types include continuous (tight junctions, e.g., muscle), fenestrated (pores, e.g., kidney), and sinusoidal (gaps, e.g., liver). Veins return blood to the heart, usually deoxygenated except for pulmonary veins. They have thinner walls than arteries due to lower pressure, with similar three layers but a prominent tunica adventitia and less tunica media. Many veins, especially in limbs, contain one-way valves to prevent backflow. Venules collect from capillaries and merge into larger veins. The venous system holds about 60–70% of total blood volume, aiding as a reservoir.

Development

Heart

The development of the heart begins in the third week of embryonic life with the formation of cardiogenic mesoderm from lateral plate mesoderm cells that migrate through the primitive streak during . These cells differentiate into cardiac progenitor cells under the influence of signaling molecules such as and inhibition of , expressing early markers like and to form the cardiac crescent. By the end of the third week (Carnegie stages 9-10), paired endothelial strands within the mesoderm canalize to form endocardial tubes, which fuse cranially to create a single primitive heart tube consisting of an outer myocardial layer, an inner endocardial layer, and intervening cardiac jelly; this tube begins primitive peristaltic contractions to initiate blood flow. In the fourth week (Carnegie stage 10-12), the straight heart tube undergoes rightward looping, transforming into a C-shaped then S-shaped structure due to differential growth rates and cytoskeletal changes in the myocardium, establishing the basic cranial-caudal and left-right axes of the future heart. This looping positions the future ventricles caudally and atria cranially, with cells from the second heart field contributing to elongation and addition of myocardium at the poles. Concurrently, chamber development emerges as ballooning of the tube walls forms primitive atrium and ventricle regions, with trabeculations—myocardial ridges—developing in the ventricles by the end of week 4 to enhance contractility and surface area. Septation of the heart occurs progressively from weeks 4 to 7 (Carnegie stages 12-18), dividing the single tube into four chambers. The atrial septum begins with the septum primum growing from the atrial roof toward the endocardial cushions in week 4, creating the ostium primum that later closes via fusion, while perforations in the septum primum form the ostium secundum; a secondary septum then overlaps it, leaving the foramen ovale as a flap-like valve. Ventricular septation starts in week 4 with the muscular septum ascending from the floor, followed by closure of the membranous portion in week 6 through fusion of atrioventricular and conotruncal cushions with contributions from neural crest cells. Outflow tract septation involves spiral-shaped endocardial cushions in weeks 6-7, separating the truncus arteriosus into aorta and pulmonary trunk. By week 8, these processes yield a four-chambered heart with partitioned atria and ventricles, integrated with emerging great vessels. Valve formation arises from endocardial cushions—swellings of cardiac jelly invaded by mesenchymal cells—in the atrioventricular canal and outflow tract during weeks 4-8 (Carnegie stages 12-23). In the atrioventricular region, cushions fuse to form the mitral and tricuspid valves through excavation and apoptosis, while semilunar valves in the outflow tract develop from three pairs of cushions that ridge and fenestrate into cusps. Fetal circulation relies on shunts that develop alongside heart formation to bypass the non-functional lungs and liver. The foramen ovale forms in week 5 as part of atrial septation, allowing oxygenated blood from the inferior vena cava to pass from the right to left atrium. The ductus arteriosus emerges in week 7 from the sixth aortic arch, connecting the pulmonary trunk to the aorta to divert blood away from the lungs. The ductus venosus, present by week 10, shunts umbilical vein blood directly to the inferior vena cava, bypassing the liver sinusoids and delivering it to the right atrium for mixing and distribution. Many congenital heart defects originate from disruptions in these developmental processes, particularly incomplete fusion during septation. Atrial septal defects (ASD) result from failure of the septum primum and secundum to fuse properly, often linked to mutations in genes like or , leading to persistent interatrial shunting. Ventricular septal defects (VSD) arise from incomplete closure of the interventricular septum, such as non-fusion of the muscular and membranous components, associated with disruptions in neural crest migration or second heart field contributions. Persistence of the foramen ovale after birth, due to inadequate fusion, creates a patent foramen ovale allowing right-to-left shunting.

Blood vessels

The embryonic development of blood vessels begins with vasculogenesis, the de novo formation of the initial vascular plexus from angioblasts derived from lateral plate mesoderm during . These angioblasts, also known as endothelial precursor cells, aggregate and differentiate into endothelial tubes that assemble into primitive blood islands, primarily in the extraembryonic yolk sac around embryonic day 7.5 in mice or week 3 in humans. This process establishes the foundational vascular network essential for nutrient distribution and oxygenation in the early embryo. Following vasculogenesis, angiogenesis drives the expansion and remodeling of the vascular system through sprouting from existing vessels, enabling the formation of a hierarchical network of arteries, veins, and capillaries. (VEGF), secreted by surrounding tissues in response to hypoxia, plays a central role by stimulating endothelial cell proliferation, migration, and filopodia extension from tip cells that guide sprout invasion into avascular regions. Other factors, such as (FGF) and angiopoietins, support lumen formation and vessel stabilization during this remodeling phase. The resulting interconnected plexus connects to the heart's outflow tracts to initiate embryonic circulation. Differentiation between arteries and veins occurs through molecular signaling that imparts distinct identities to endothelial cells within the angiogenic network. Ephrin-B2 and its receptor EphB4 are key mediators, with ephrin-B2 expressed in arterial endothelium promoting repulsive interactions that segregate arterial and venous domains, while EphB4 marks venous endothelium. Notch signaling further reinforces arterial fate by upregulating arterial-specific genes and suppressing venous markers. Concurrently, smooth muscle cells, derived from neural crest or mesoderm, are recruited to the abluminal surface of vessels—predominantly arteries—via platelet-derived growth factor (PDGF) signaling from endothelium, providing structural support and vasoregulatory function. In the fetus, the yolk sac and placenta make critical contributions to vascular development and early circulation. The yolk sac, originating from the hypoblast, undergoes vasculogenesis to form vitelline vessels that facilitate initial materno-fetal nutrient exchange before placental dominance. These extraembryonic vessels connect to the intraembryonic circulation, supporting hematopoiesis and oxygenation until approximately week 8 in humans. The placental vasculature, developing from chorionic mesoderm, expands through both vasculogenesis and angiogenesis to create a low-resistance fetoplacental circulation vital for fetal growth and gas exchange. Vascular maturation involves the acquisition of innervation and sensory structures to enable autonomic control and pressure sensing. Sympathetic and parasympathetic nerves extend along developing vessels from neural crest-derived ganglia, influencing vasoconstriction and vasodilation through neurotransmitter release, with patterning guided by vascular cues like semaphorins. Baroreceptors, mechanosensitive endings in the carotid sinus and aortic arch walls, emerge during late gestation, maturing to detect pressure changes and elicit reflex adjustments in heart rate and vascular tone, with sensitivity increasing progressively toward birth. This innervation and baroreflex development integrate the vascular system into broader cardiovascular regulation.

Function

Physiological roles

The circulatory system plays a central role in gas exchange by transporting oxygen from the lungs to tissues and carbon dioxide from tissues to the lungs. Approximately 98% of oxygen in arterial blood is bound to hemoglobin in red blood cells, forming oxyhemoglobin, while the remainder is dissolved in plasma. The oxyhemoglobin dissociation curve, which has a sigmoid shape, enables efficient oxygen loading in the oxygen-rich pulmonary capillaries and unloading in oxygen-poor peripheral tissues, influenced by factors such as pH, temperature, and 2,3-diphosphoglycerate levels. Carbon dioxide is transported primarily as bicarbonate ions (about 70-90%), with smaller portions dissolved in plasma or bound to hemoglobin as carbaminohemoglobin. Beyond gases, the circulatory system delivers essential nutrients, such as and , to cells via the bloodstream, supporting metabolic processes. It also facilitates the removal of metabolic wastes, including from protein breakdown and from anaerobic metabolism, directing them to excretory organs like the kidneys and liver. secreted by endocrine glands, such as and , are distributed throughout the body to regulate physiological functions like metabolism and growth. Additionally, the system enables immune cell trafficking by carrying and to sites of infection or injury, aiding in defense against pathogens. The circulatory system contributes to temperature regulation through blood flow adjustments; vasodilation in skin vessels promotes heat loss via radiation and convection, while vasoconstriction conserves heat by reducing peripheral flow. In homeostasis, it maintains pH balance primarily through the , which neutralizes acids and bases in blood, and by transporting CO2 to the lungs for elimination. Fluid volume is controlled at capillary exchange sites via , where hydrostatic pressure drives fluid out and oncotic pressure pulls it back, preventing edema and ensuring stable blood volume. To meet metabolic demands, the heart pumps blood at a resting cardiac output of 5-6 liters per minute in adults, delivering oxygen and nutrients proportional to tissue needs; this increases substantially during exercise to support elevated energy expenditure.

Circulatory pathways

The circulatory system features distinct pathways that direct blood flow to facilitate gas exchange, nutrient delivery, and waste removal. Pulmonary circulation begins in the right ventricle, where deoxygenated blood is pumped through the pulmonary trunk and arteries to the lungs for oxygenation via gas exchange in the . This low-pressure system, with mean pulmonary arterial pressure of approximately 14 mmHg (range 9-18 mmHg), contrasts with systemic circulation and minimizes the workload on the right heart while allowing efficient oxygen uptake. Oxygenated blood then returns via pulmonary veins to the left atrium. Systemic circulation originates from the left ventricle, ejecting oxygenated blood into the at high pressure—typically systolic pressures around 120 mmHg—to distribute it throughout the body. The branches into major arteries such as the brachiocephalic, left common carotid, and left subclavian from the aortic arch, followed by descending branches like the renal and mesenteric arteries that supply organs including the kidneys, intestines, and limbs. This high-pressure pathway ensures adequate perfusion to peripheral tissues despite resistance from narrower vessels. Specialized circulations adapt these pathways for specific organs. The coronary circulation supplies the myocardium with oxygenated blood via arteries branching from the aorta's base, delivering about 5% of cardiac output to meet the heart's high metabolic demands. Cerebral circulation maintains brain homeostasis through a network of arteries like the carotids and vertebrals, protected by the formed by endothelial cells that selectively regulate substance passage to shield neural tissue. Renal circulation directs blood to the kidneys for filtration, with afferent arterioles feeding glomeruli where plasma is filtered to form urine precursors, accounting for roughly 20% of cardiac output. The hepatic portal system routes nutrient-rich, deoxygenated blood from the gastrointestinal tract and spleen directly to the liver via the portal vein for processing and detoxification before entering systemic circulation. In fetuses, temporary shunts like the and bypass the non-functional lungs and liver, redirecting oxygenated blood from the placenta to vital organs until birth. Hemodynamics governs blood flow dynamics across these pathways, with pressure, velocity, and resistance varying by vessel type. Arterial pressure exhibits systolic peaks during ventricular contraction (around 120 mmHg) and diastolic troughs during relaxation (around 80 mmHg), dropping progressively from large arteries (mean ~100 mmHg) to capillaries (~25 mmHg) due to frictional losses and branching. Blood velocity decreases markedly from arteries (~50 cm/s) to capillaries (~0.03 cm/s), reflecting the inverse relationship with total cross-sectional area, which maximizes exchange time in microvessels. Peripheral resistance, primarily in arterioles, opposes flow and is quantified by :
R = \frac{8 \eta L}{\pi r^4}
where R is resistance, \eta is blood viscosity, L is vessel length, and r is radius; small radius changes dramatically affect resistance, enabling local flow regulation. Overall cardiac output, the volume pumped per minute, is calculated as:
CO = SV \times HR
where SV is stroke volume (~70 mL) and HR is heart rate (~70 beats/min), yielding ~5 L/min at rest to sustain both pulmonary and systemic demands.

Regulation

The circulatory system's regulation maintains blood pressure, flow distribution, and oxygen delivery through integrated neural, hormonal, and local mechanisms. These controls enable rapid adjustments to physiological demands, such as exercise or posture changes, while ensuring long-term homeostasis. The autonomic nervous system provides primary short-term neural control via its sympathetic and parasympathetic branches. Sympathetic activation, mediated by norepinephrine release from postganglionic fibers, increases heart rate and contractility while inducing vasoconstriction in most vascular beds to elevate blood pressure. In contrast, parasympathetic stimulation through vagal nerves releases acetylcholine, primarily slowing heart rate (bradycardia) to reduce cardiac output and blood pressure during rest. These opposing influences allow fine-tuned responses, with sympathetic dominance promoting "fight-or-flight" states and parasympathetic fostering "rest-and-digest" recovery. Hormonal mechanisms contribute to both acute and sustained regulation, particularly via the renin-angiotensin-aldosterone system (RAAS). Low renal perfusion triggers renin release from juxtaglomerular cells, converting angiotensinogen to angiotensin I, which is then cleaved to angiotensin II by angiotensin-converting enzyme; angiotensin II causes systemic vasoconstriction and stimulates aldosterone secretion to promote sodium and water retention, thereby increasing blood volume and pressure. Antidiuretic hormone (ADH, or vasopressin) from the posterior pituitary enhances vasoconstriction and renal water reabsorption in response to high osmolarity or hypotension. Counterbalancing these, atrial natriuretic peptide (ANP), secreted by cardiac atrial cells during volume expansion, induces natriuresis, diuresis, and vasodilation to lower blood pressure. Local autoregulation ensures tissue-specific blood flow stability independent of systemic changes, primarily through myogenic responses and metabolic factors. Vascular smooth muscle contracts in response to increased transmural pressure (), constricting arterioles to maintain constant flow, as demonstrated in renal and cerebral circulations where pressure rises from 80 to 130 mmHg reduce flow increments by up to 50%. Metabolites like , produced by endothelial cells, promote vasodilation to match oxygen demand, while adenosine accumulation during hypoxia or ischemia further relaxes vessels to enhance local perfusion. Baroreceptors and chemoreceptors serve as key sensors in reflex arcs. Baroreceptors in the carotid sinus and aortic arch detect stretch from arterial pressure changes, relaying signals via the glossopharyngeal and vagus nerves to the brainstem's cardiovascular center; high pressure activates parasympathetic output and inhibits sympathetic activity to lower pressure, while low pressure does the opposite. Adjacent chemoreceptors in the carotid and aortic bodies monitor blood pH, oxygen, and carbon dioxide levels, stimulating sympathetic responses during hypoxia or hypercapnia to increase ventilation and cardiac output. Feedback loops integrate these elements for dynamic control, distinguishing short-term neural from long-term renal pathways. Short-term neural loops, like the , rapidly adjust heart rate and vessel tone within seconds to minutes via autonomic efferents. Long-term renal loops, involving and pressure natriuresis, sustain blood volume and pressure over hours to days by modulating sodium excretion and fluid balance in response to chronic perturbations. These loops interact, with neural inputs influencing renal function to prevent sustained deviations from homeostasis.

Clinical significance

Cardiovascular diseases

Cardiovascular diseases (CVDs) encompass a group of disorders affecting the heart and blood vessels, representing the leading cause of death worldwide, with an estimated 19.8 million fatalities in 2022. These conditions often stem from shared risk factors such as high blood pressure, elevated cholesterol, smoking, diabetes, and obesity, which promote vascular damage and impair circulatory function. Atherosclerosis, a foundational process in many CVDs, involves the buildup of fatty plaques in arterial walls, leading to narrowing and hardening that restricts blood flow and heightens the risk of ischemia. Key risk factors for atherosclerosis include hyperlipidemia, hypertension, cigarette smoking, and diabetes mellitus, which collectively accelerate plaque formation and endothelial dysfunction. Complications arise when plaques rupture, triggering thrombosis that can cause acute events like myocardial infarction or stroke. Hypertension, or persistently elevated blood pressure, is classified as primary (essential, affecting 90-95% of cases with no identifiable cause) or secondary (due to underlying conditions like renal disease). It imposes chronic stress on the cardiovascular system, resulting in complications such as , heart failure, coronary heart disease, and chronic kidney disease. Heart failure occurs when the heart cannot pump blood effectively to meet the body's needs, categorized as systolic (impaired contraction with reduced ejection fraction typically below 40%) or diastolic (preserved ejection fraction but stiff ventricles hindering filling). Systolic heart failure often follows from , while diastolic variants are linked to hypertension and aging. Arrhythmias disrupt the heart's electrical rhythm, with (AFib) being the most common sustained type, characterized by irregular atrial contractions that increase stroke risk through clot formation. Ventricular tachycardia involves rapid ventricular beats exceeding 100 per minute, potentially degenerating into life-threatening fibrillation if sustained. Valvular heart diseases impair valve function through stenosis (narrowing) or regurgitation (leakage), accounting for 10-20% of cardiac surgical cases and often resulting from degenerative changes, infections, or congenital defects. Aneurysms manifest as localized arterial dilations, particularly in the aorta, where wall weakening from atherosclerosis or hypertension risks rupture and hemorrhage. (PAD) entails atherosclerotic narrowing of limb arteries, causing claudication and elevating amputation risk in advanced stages. Post-2020, long COVID has emerged as a contributor to vascular pathologies, with persistent endothelial damage from SARS-CoV-2 infection promoting inflammation, thrombosis, and microvascular injury even months after acute illness. This endothelial dysfunction, evidenced by reduced flow-mediated dilation, heightens susceptibility to clots and ongoing cardiovascular complications in affected individuals. Studies indicate that such vascular sequelae may underlie symptoms like fatigue and dyspnea in long COVID, linking acute infection to chronic circulatory impairment.

Diagnostic investigations

Diagnostic investigations of the circulatory system encompass a range of non-invasive, imaging, laboratory, and invasive techniques designed to evaluate cardiac structure, function, blood flow, and risk factors for cardiovascular disease. These methods allow clinicians to detect abnormalities such as arrhythmias, valvular dysfunction, coronary artery disease, and heart failure, guiding appropriate management. Selection of tests depends on patient symptoms, risk profile, and clinical context, with guidelines from organizations like the emphasizing a stepwise approach starting with non-invasive assessments. Non-invasive techniques form the cornerstone of initial evaluation. Blood pressure monitoring, a fundamental assessment, measures systolic and diastolic pressures to identify hypertension, a major risk factor for circulatory disorders; ambulatory monitoring over 24 hours provides a comprehensive profile of variability and nocturnal patterns. The electrocardiogram (ECG) records the heart's electrical activity to detect arrhythmias, ischemia, or conduction abnormalities, with a standard 12-lead ECG capturing data in about 10 seconds for routine screening. Holter monitors extend this by providing continuous 24- to 48-hour ECG recordings to capture intermittent events like atrial fibrillation in ambulatory patients. Echocardiography uses ultrasound to visualize heart chambers, valves, and wall motion, while Doppler echocardiography assesses blood flow velocity and direction, quantifying regurgitant fractions or stenosis severity in real time without radiation exposure. Imaging modalities offer detailed anatomical and functional insights. Carotid ultrasound measures intima-media thickness (IMT), a non-invasive marker of subclinical atherosclerosis where increased thickness (>0.9 mm) predicts cardiovascular events independently of traditional risk scores. Angiography, often coronary angiography, visualizes vessel lumens via contrast injection to identify stenoses or occlusions, serving as a gold standard for coronary artery disease assessment. Computed tomography (CT) angiography provides 3D mapping of coronary arteries with high spatial resolution, detecting calcifications and plaques non-invasively, while cardiac magnetic resonance imaging (MRI) excels in tissue characterization, perfusion assessment, and viability evaluation without ionizing radiation. Laboratory tests analyze components to identify risk factors and acute events. Lipid profiles measure total , LDL, HDL, and triglycerides to stratify atherosclerotic risk, with elevated LDL (>160 mg/dL) indicating need for intervention per guidelines. levels, highly sensitive biomarkers, rise within hours of , confirming cardiac injury with serial measurements showing peak values around 24 hours. B-type (BNP) or NT-proBNP assays detect by quantifying ventricular strain, with levels >100 pg/mL suggesting congestion and guiding prognosis. Invasive procedures are reserved for definitive diagnosis when non-invasive tests are inconclusive. involves inserting a via femoral or to measure intracardiac pressures, oxygen saturations, and perform ventriculography, directly assessing shunts or gradients in complex cases. , including exercise or pharmacologic variants, evaluates myocardial ischemia by monitoring ECG changes, , and symptoms under controlled workload, with ST-segment depression indicating coronary insufficiency. Recent advances have integrated technology for enhanced accessibility and precision. Wearable devices, such as smartwatches with photoplethysmography, detect through irregular pulse notifications, achieving sensitivities of 85-98% in validation studies and enabling early intervention in asymptomatic individuals. Artificial intelligence in ECG interpretation, particularly algorithms approved post-2023, improves detection of subtle patterns like low or silent ischemia, with convolutional neural networks outperforming traditional methods in large cohorts by reducing false negatives by up to 20%.

Surgical interventions

Surgical interventions for circulatory system disorders aim to restore optimal blood flow, repair structural defects, and support cardiac function in patients with conditions such as , valvular dysfunction, , and vascular aneurysms. These procedures range from traditional open surgeries to advanced minimally invasive and endovascular techniques, with selection guided by factors including lesion complexity, patient comorbidities, and anatomical suitability. Post-2023 advancements have emphasized catheter-based and robotic approaches to reduce recovery times and risks while maintaining efficacy comparable to open surgery. Coronary artery bypass grafting (CABG) treats multivessel by harvesting a saphenous vein or internal mammary artery graft to reroute blood around atherosclerotic blockages, thereby alleviating ischemia. Performed via under or off-pump, CABG improves long-term survival in patients with left main or three-vessel disease, with five-year patency rates exceeding 85% for arterial grafts. Percutaneous coronary intervention (PCI) with angioplasty and drug-eluting stents (DES) provides a catheter-based alternative for focal coronary stenoses, involving balloon dilation followed by deployment to scaffold the vessel and elute antiproliferative agents like , which inhibit neointimal . have lowered revascularization rates to 5-10% at one year, compared to 20-30% with bare-metal stents, particularly benefiting diabetic patients. Valve repair or replacement addresses regurgitation or , with (TAVR) emerging as a frontline option for severe in intermediate- to low-risk patients. Delivered transfemorally, TAVR deploys a balloon- or self-expanding bioprosthetic valve within the native annulus, achieving procedural success rates over 95% and reducing all-cause mortality versus medical therapy alone. Surgical repair techniques, such as annuloplasty for , preserve native tissue and yield durable results in younger cohorts. Heart transplantation serves as the gold standard for irreversible end-stage , involving orthotopic replacement of the donor heart with meticulous of major vessels and atria. Post-transplant, lifelong mitigates rejection, yielding one-year survival rates of 85-90% and median graft survival of 12 years, though chronic allograft vasculopathy remains a leading cause of late failure. Ventricular assist devices, particularly left ventricular assist devices (LVADs), mechanically unload the failing ventricle by pumping blood from the left atrium or ventricle to the , used as bridges to transplant or permanent . Continuous-flow LVADs like the HeartMate 3 demonstrate two-year survival rates of 70-80% in destination , with reduced incidence due to improved hemocompatibility. Endovascular repairs target aneurysmal or occlusive peripheral vascular disease; for abdominal aortic aneurysms, endovascular aneurysm repair (EVAR) deploys a modular stent-graft to seal the sac, lowering 30-day mortality to 1-2% versus 4-5% for open repair. Peripheral bypass surgery employs autologous vein or prosthetic grafts to bypass femoropopliteal occlusions, achieving primary patency rates of 70-80% at five years for above-knee procedures. Robotic-assisted surgery has advanced minimally invasive cardiac interventions since 2023, utilizing systems like the da Vinci platform for precise endoscopic manipulation in procedures such as coronary and valve repairs, resulting in shorter hospital stays (median 4-5 days) and lower transfusion needs compared to sternotomy. 2024-2025 updates include enhanced haptic feedback and integration for intraoperative guidance, expanding adoption for complex multivessel . Gene therapy trials for vascular repair, updated through 2025, explore CRISPR-Cas9 editing to correct mutations in genes like those encoding vascular endothelial growth factors, aiming to enhance endothelial regeneration and avert restenosis in . Phase I/II studies, such as those targeting familial hypercholesterolemia-related vasculopathy, report preliminary safety with no major adverse events at one-year follow-up, though endpoints remain under evaluation. Complications of these interventions include restenosis, affecting 5-10% of cases despite and up to 15% of vein grafts in CABG at five years, often necessitating repeat procedures. Infection rates vary, with sternal wound post-CABG occurring in 1-5% of patients, associated with factors like and , and carrying a 20-30% mortality risk if . Endovascular approaches like EVAR exhibit lower overall rates (under 1%) but risk endoleaks leading to rupture in 10-20% over time.

Other animals

Open circulatory systems

In an open circulatory system, the circulatory fluid known as hemolymph is pumped by a heart into the body cavity, where it directly bathes the tissues and organs to facilitate nutrient and gas exchange, before draining back into the heart through specific openings. This contrasts with closed systems by lacking a continuous network of enclosed vessels, allowing hemolymph to serve both as blood and interstitial fluid. Key components include a muscular heart that propels hemolymph, ostia as valved openings in the heart walls that permit unidirectional entry of hemolymph during diastole, and a limited set of vessels such as arteries that distribute fluid into open sinuses or the hemocoel. Accessory pulsatile organs, often located in the head, thorax, or appendages, assist the primary heart by providing localized pumping to enhance flow in specific regions. The system operates at low pressure, typically generating systolic pressures below 20 mmHg in many species, which supports passive diffusion across tissues. Open circulatory systems are prevalent in , particularly arthropods such as , where the dorsal vessel functions as both heart and , extending longitudinally through the and to pump anteriorly. In most mollusks, including bivalves and gastropods, circulates through a hemocoel with a multi-chambered heart, though cephalopods like squid represent an exception with a adapted for higher activity levels. Arthropods like crustaceans also feature open systems, with filling the hemocoel after leaving short arteries from the dorsal heart. The simplicity of open systems offers advantages, including reduced structural complexity and lower energy expenditure for circulation, making them suitable for small-bodied organisms with modest metabolic demands. This energy efficiency arises from the low-pressure operation, which minimizes the work required by the heart compared to high-pressure closed systems. However, limitations include inefficient and oxygen delivery due to reliance on in the hemocoel, which restricts the system to organisms with low oxygen requirements and constrains body size in active or larger species. The sluggish flow and lack of precise control can hinder rapid responses to physiological needs in environments demanding high metabolic rates.

Closed circulatory systems

A closed circulatory system is characterized by blood being confined within a continuous network of vessels, distinct from the surrounding interstitial fluid, and pumped by a muscular heart to facilitate throughout the body. This arrangement is prevalent in all vertebrates and select , including annelids like and cephalopods such as octopuses, where it enables precise control over fluid distribution. Unlike systems where fluid bathes tissues directly, the vascular confinement here maintains separation, allowing for specialized functions in , gas, and waste exchange. In vertebrates, closed systems exhibit variations in circuit complexity adapted to environmental and metabolic demands. Fish possess a single-circuit system, where deoxygenated blood flows from the two-chambered heart to the gills for oxygenation, then directly to the body before returning to the heart, supporting aquatic respiration efficiently but limiting pressure in systemic circulation. Amphibians and most reptiles feature a double-circuit system with a three-chambered heart (two atria and one ventricle), directing blood through pulmonary or pulmocutaneous pathways for gas exchange and a systemic circuit for tissue perfusion, though partial mixing of oxygenated and deoxygenated blood occurs due to the shared ventricle. Birds and mammals, in contrast, have a fully separated double-circuit system powered by a four-chambered heart (two atria and two ventricles), ensuring oxygenated blood from the lungs reaches the body under high pressure via the systemic circuit, while deoxygenated blood returns separately for pulmonary recirculation; this separation evolved independently in both lineages to meet high metabolic needs. The primary advantages of closed circulatory systems lie in their capacity to generate and sustain higher hydrostatic pressure compared to open systems, which propels rapidly through vessels for efficient and oxygen delivery to distant tissues. This high-pressure mechanism supports larger body sizes, elevated metabolic rates, and active lifestyles in vertebrates, as seen in endothermic and mammals that require consistent oxygen supply for sustained activity. Key components include endothelial cells lining all vessels, forming a semi-permeable barrier that prevents leakage into tissues while regulating permeability; this lining is particularly thin in capillaries, where it facilitates of gases, nutrients, and wastes between and cells without direct mixing. In specialized vascular beds like those in the liver or , the endothelium allows controlled exchange akin to open systems but within a closed .

Systems without circulation

Organisms lacking a dedicated circulatory system rely on passive and body movements to oxygen, nutrients, and products across their tissues. In these systems, substances move directly from areas of high concentration to low concentration without the aid of specialized vessels or pumps, enabling adequate exchange in simple body plans. Key mechanisms facilitating this transport include a high surface-to-volume ratio, which minimizes the distance molecules must diffuse, and the use of fluids such as pseudocoel or fluids to aid distribution. For instance, sponges (phylum Porifera) employ choanocytes—flagellated collar cells—to generate water currents through their porous bodies, allowing nutrients and gases to diffuse across cell layers into the , a gel-like matrix. Similarly, flatworms like (phylum Platyhelminthes) maintain a flattened that enhances diffusion efficiency, with nutrients absorbed directly from the gastrovascular cavity and distributed via body undulations. Cnidarians, such as jellyfish (phylum Cnidaria), utilize their gastrovascular cavity for both digestion and nutrient circulation, where body contractions facilitate mixing and diffusion to surrounding tissues. These diffusion-based systems impose significant limitations, primarily constraining organisms to small sizes—typically under 1 mm in thickness—to ensure timely , and supporting only low metabolic rates that do not demand rapid delivery of resources. Larger or more active forms would face inefficiencies, as diffusion rates decrease with distance, leading to potential in deeper tissues. Evolutionarily, such systems are characteristic of basal metazoans, including poriferans, cnidarians, and early triploblastic animals like flatworms, which represent primitive adaptations predating the emergence of vascularized circulation over 600 million years ago. This reliance on reflects an ancestral strategy for multicellular life before the selective pressures for in more complex lineages.

History

Early concepts

In ancient Egypt, medical knowledge documented in the Ebers Papyrus, dating to approximately 1550 BCE, described the body as interconnected by 22 metu, or vessels, that served as channels for blood and the vital force sustaining life, with the heart positioned as the central organ from which these vessels extended to all parts of the body. This view emphasized the heart's role in distributing metu, linking physical health to the flow of these essential substances, though without recognition of a closed circulatory loop. Among the ancient and Romans, , active in the BCE, developed the theory of the four humors—, , yellow , and black —positing that health depended on their balance within the body, with as one key fluid influencing vitality but not yet conceptualized as circulating systemically. This humoral framework laid groundwork for later physiological ideas, though it treated more as a static essence than a dynamic flow. In the 2nd century CE, of advanced a more detailed but flawed model of circulation, asserting that the liver generated nutrient-rich distributed through veins to the right side of the heart, while arteries carried —a vital spirit derived from air—originating from the left heart after passed through invisible pores in the from right to left, with lungs facilitating infusion rather than full oxygenation. 's system, influential for over a millennium, erroneously separated venous and arterial functions without acknowledging recirculation. During the , Islamic scholar (Ibn Sina) perpetuated and refined Galenic physiology in his , completed in 1025 CE, where he cited extensively—over 300 times—while integrating Aristotelian elements, maintaining the liver-heart-lung pathway for blood and distribution as the core mechanism of bodily nourishment and respiration. This text reinforced Galen's errors across and the , emphasizing humoral balance and vessel-based transport without empirical challenges to the non-circulatory model. Renaissance anatomists began challenging ancient doctrines through direct observation. Andreas Vesalius, in his 1543 work De Humani Corporis Fabrica, detailed human dissections that corrected Galenic inaccuracies, such as the number and structure of heart valves and vessel origins, promoting reliance on empirical anatomy over textual authority, though he still adhered to a non-circulatory view of blood flow. Building on this, Hieronymus Fabricius ab Aquapendente described the semilunar valves in veins in his 1603 treatise De Venarum Ostiolis, noting their role in directing blood flow toward the heart and preventing reflux, a discovery that hinted at directional circulation without fully explaining its mechanism. In parallel ancient traditions, Chinese medicine, as outlined in the around 200 BCE, conceptualized —vital energy—as flowing through meridians to regulate blood circulation within vessels, with the heart governing this harmonious interplay to maintain health, distinct from Western humoral models by emphasizing energetic balance over fluid production. Similarly, in Indian Ayurveda, texts like the Ashtanga Hridaya by (7th century CE) described , the life force, as propelled by vayus such as in the heart for intake and for systemic distribution of rasa (plasma) and rakta (), viewing circulation as an energetic tied to doshic rather than mechanical pumping.

Key discoveries

In 1628, published De Motu Cordis, demonstrating that blood circulates in a closed loop driven by the heart's pumping action, overturning the prevailing view of blood flowing unidirectionally from the liver to the body. Harvey's quantitative experiments estimated the total in humans to be around 5 liters, far exceeding prior assumptions, and showed that the heart's output could not be replenished solely by , thus necessitating recirculation. Advancements in microscopy in the mid-17th century revealed key microstructures of the circulatory system. In 1661, Marcello Malpighi identified capillaries in the lungs and frog skin using early microscopes, providing direct evidence of the connections between arteries and veins that Harvey had inferred, completing the description of the closed circulatory loop. A decade later, in 1674, Antonie van Leeuwenhoek observed red blood cells and their flow through capillaries in fish tails and tadpole tails, offering the first visual confirmation of blood as a cellular fluid rather than a homogeneous humor. The brought quantitative and physiological insights into blood flow and . In the 1840s, developed the law of in tubes, applying it to blood vessels to describe how pressure, radius, and viscosity govern flow rates, laying the foundation for . Toward the century's end, Ernest Henry Starling's work in the 1890s elucidated the role of lymphatics in , with his experiments showing how hydrostatic and oncotic pressures regulate capillary and , as formalized in Starling's hypothesis. In 1903, invented the string galvanometer for electrocardiography (ECG), enabling non-invasive recording of the heart's electrical activity, for which he received the in or in 1924. The 20th century saw transformative clinical breakthroughs in circulatory interventions. In the 1950s, developed the heart-lung machine, enabling the first successful open-heart surgery in 1953 by temporarily bypassing the heart and lungs, revolutionizing cardiac procedures. Building on this, in 1977, Andreas Grüntzig performed the first percutaneous transluminal coronary angioplasty (PTCA), using a to widen narrowed arteries without open surgery, marking the advent of minimally invasive vascular treatments. Modern discoveries have delved into molecular and genetic regulation of the circulatory system. In 1989, Napoleone Ferrara and colleagues isolated (VEGF), identifying it as a key signaling protein that promotes and , with profound implications for understanding and treating vascular diseases. Post-2023 advancements in have enhanced circulatory modeling, with algorithms simulating complex and predicting cardiovascular risks from imaging data, as validated in large-scale studies integrating with 4D flow MRI.