Clinical Significance
Human serum albumin is a basic laboratory measurement in clinical medicine and is transfused as a colloid fluid. In the laboratory, bovine serum albumin is used as a laboratory standard.[5][6][7]
Serum Albumin as a Laboratory Test
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The liver’s biosynthetic capacity or, in other words, a patient’s liver functioning can be measured by drawing their serum albumin. Albumin is often coupled with a prothrombin time or international normalized ratio to more fully assess liver biosynthesis. However, serum albumin values can be normal in states of chronic liver disease and abnormal in cases of normal liver function. A review of patients undergoing evaluation for gastric bypass, liver pathology, and liver function tests correlated poorly. Further, hypoalbuminemia can reflect decreased albumin synthesis or a decrease in concentration relative to the free fluid. The latter state of hypoalbuminemia can be seen in cases of hepatic failure with ascites, as well as renal or congestive heart failure. Thus, the patient’s clinical context must be considered during the evaluation and diagnostic workup.
Some patients who are malnourished have hypoalbuminemia or low serum albumin levels. The effects of fasting can have a rapid onset, leading to a one-third decrease in albumin within 24 to 48 hours of fasting onset. However, this reverses quickly with replenishment, restoring the liver’s ability to synthesize albumin within 15 to 30 minutes. Since malnourishment has been associated with adverse events in the post-surgical period, it is commonly used as a clinical measure for nutritional optimization and readiness for surgery. Albumin is 1 of many laboratory measurements utilized to evaluate a patient’s nutritional status. Other laboratory measurements include pre-albumin, transferrin, and retinol-binding protein. However, none of these laboratory measurements stand alone and must be combined with a physical examination of the patient. Hypoalbuminemia is also useful for the diagnosis and monitoring of patients with anasarca and malabsorption.
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Albumin levels can fall in patients with inflammatory disorders and other conditions. This may be due to the liver’s downregulated production of albumin mRNA, leading to reduced synthesis, increased albumin catabolism, and increased vascular permeability.[8]
Albumin has additional utility in diagnosing patients with fluid accumulation in the peritoneum or ascites. Ascites can occur for a wide variety of reasons, including congestive heart failure, liver failure, and malignancy. A clinician can perform a diagnostic paracentesis to drain ascitic fluid, compare the albumin in this fluid to serum albumin levels, and calculate a serum ascites-albumin gradient (SAAG).
A SAAG of 1.1 or greater suggests ascites secondary to a portal hypertensive etiology such as congestive heart failure, hepatic cirrhosis, and alcoholic hepatitis. A SAAG of less than 1.1 indicates ascites of a non-portal hypertensive etiology, such as peritoneal carcinomatosis, Mycobacterium tuberculosis, nephrotic syndrome, pancreatitis, and serositis.
Serum Albumin as a Colloid Fluid
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The clinical use of the colloid fluid, albumin, in critically ill patients is a topic of debate. Some clinicians advocate using albumin because it remains intravascular for longer than crystalloids and theoretically leads to less pulmonary edema. However, the benefits of albumin over crystalloids, such as lactated ringers and normal saline, have not been proven in trials. Furthermore, the clinician must consider the relatively higher cost of albumin than crystalloids. When treating hypovolemic shock, the first consideration is, “What is the patient losing?” If they are in shock secondary to hemorrhage from a gunshot wound, for example, packed red blood cells are of greatest importance. However, albumin is theoretically advantageous over crystalloids for its potential to increase a patient’s oncotic pressure. Its short half-life limits the effects of albumin.
As mentioned above, the strength of albumin over crystalloids is that it increases intravascular oncotic pressure. There are some situations where a patient needs improved oncotic pressure, which can be advantageous. In cirrhotic patients receiving large volumes (more than 5 liters) of paracenteses, giving the patient 6g to 8g of albumin for each liter of ascetic fluid drained could lead to less incidence of hemodynamic compromise. However, a recent systematic review concluded that in cirrhotic patients without hepatocellular carcinoma, there is no mortality benefit to administering albumin after large-volume paracentesis. More studies are needed to confirm or refute this finding.
Serum Albumin and Wound Complications in Orthopedic Surgery
Surgical site infection (SSI) is an unfortunately common postoperative complication encountered throughout the entire field of orthopedic surgery (eg, orthopedic spine surgery, elective total joint replacement, orthopedic trauma cases). Serum albumin <3.5 g/dL has been demonstrated to confer an increased risk of SSI following these procedures. Especially in elective THA and TKA procedures, which demonstrate a wide range of reproducibility and success regarding positive short- and long-term outcomes in appropriately selected patients, patient malnutrition status is often considered when performing these procedures.[9][10][11][12]
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