Blood Management and Complex Spine Surgery

Summary of Key Points

Blood transfusion is no longer driven by the “10/30 hemoglobin/hematocrit rule,” because as little as one unit of homologous blood transfusion can increase postoperative complications. Therefore, a more restrictive transfusion protocol has become the standard of care.
More than 50 drugs are approved that interfere with either the coagulation cascade or platelet function. Table 84.1 lists many of these drugs and gives useful data on managing these medications. Reversal agents for anticoagulants, where present, are noted in the table.
Autotransfusion of autologous blood scavenged during surgery (“cell-saver”) can lessen the need for homologous blood transfusion.
Patient positioning using dedicated spine operating tables and hypotensive anesthesia techniques, when appropriate, lessen blood loss by reducing venous pressure, resulting in less epidural bleeding and less overall blood loss.
The coagulation cascade can be manipulated by local or systemic agents to lessen surgical blood loss, with transexamic acid being the most commonly used systemic agent.
Potential operative blood loss should be calculated before surgery, blood products should be made available, and communication with the surgical team should include transfusion triggers and the clotting status of the patient. Mass transfusion protocols are available for cases of extreme blood loss.

Minimizing blood loss in spine surgery increases safety and improves patient outcomes. The causes for significant operative blood loss may be divided into two primary categories, which can cascade together, worsening blood loss. These are patient factors (e.g., habitus, epidural vascular anatomy, coagulation characteristics) and technical factors (e.g., number of levels, dissection technique, hemostatic control). Optimal mitigation of patient factors usually occurs before the date of surgery by modifying factors like body weight and normalizing the patient’s coagulation profile (i.e., holding anticoagulants or medications and supplementals that affect bleeding or working with a hematologist to address chronic anemia and/or coagulation deficiencies). Conversely, the impact of technical factors is greatest in the immediate perioperative period. Blood loss and transfusion requirements are significantly affected by surgical technique, including duration of surgery, attention to hemostatic control, patient positioning, anesthetic techniques, and the pharmacological agents used during surgery. Managing blood loss involves rational planning before and throughout the perioperative period, through attentive manipulation of these two primary factors. A well thought-out plan for managing blood loss will incorporate measures to optimize the clotting cascade, minimize intraoperative blood loss, and plan for the replacement of blood products through intraoperative blood salvage or, in some cases, transfusion. This chapter briefly reviews the physiology of hemostasis and then catalogs interventions available to the spine surgeon that can address these patient and technical factors so as to optimize hemostatic management.

Brief Review of Surgical Hemostasis

Surgical hemostasis is the controlled arrest of bleeding through physiological (i.e., coagulation) and physical methods (i.e., ligation). The primary physiology at play in hemostasis is clot formation, which is a complex pathway of interconnected reactions. Reducing this complex system to its basic steps allows key components to be assessed with an aim toward improved hemostatic control. The first key step in this process is platelet activation, which occurs in response to exposed collagen in injured endothelium, thrombin, thromboxane A2, or adenine diphosphate. The hemostatic plug, which forms in response to platelet activation in areas of endothelial injury, is termed primary hemostasis. Secondary hemostasis refers to the activation of the coagulation cascade, which ultimately produces a fibrin clot. As hemostasis progresses and a fibrin clot is formed, the fibrinolytic system is simultaneously activated to start the process of clot lysis (tertiary hemostasis) and thereby maintain a balance between clot formation and lysis. Critical to surgical hemostasis is the surgeon’s recognition of factors that will inhibit platelet function, thereby decreasing the effectiveness of primary hemostasis, as well as factors that inhibit the coagulation cascade, which in turn decreases secondary hemostasis. In addition, to physiological methods, physical methods in terms of timely vessel ligation, (electro) coagulation or tamponade, and the reduction of hydrostatic pressure in the epidural system are also measures at the control of the surgical team, which can result in less surgical blood loss.

Preoperative Evaluation

A key component of the patient evaluation for spine surgery is a complete medical history. Special attention should be paid to medication history, as many medications interfere with primary and secondary hemostasis. Likewise, disease states such as renal failure, hematological conditions, collagen disorders, and liver disease also affect hemostasis. These medical conditions should be diagnosed and optimized before surgery if possible. Patients with uncorrectable medical issues may be too ill for elective spine surgery, and clinical judgment will be required to balance the risks versus benefits. A chemistry panel will yield information on renal and hepatic function and may be useful for evaluation in specific patients. In patients with a personal or family history of bleeding disorder or those who report easy bruising, nose bleeds, menorrhagia, multiple miscarriages, or excessive blood loss with prior surgical procedures, a coagulation profile with coagulation times, platelet counts, and, in some instances, platelet function testing or a thromboelastogram should be obtained.

Preoperative anemia with hemoglobin (Hgb) levels less than 12 g/dL are associated with increased blood transfusion requirements and should be addressed if significant surgical blood loss is anticipated. Preoperative anemia may be treated with erythropoietin in combination with iron supplementation therapy and hematologist consultation. Consideration should be given to delaying elective surgical cases until the Hgb level exceeds 12 g/dL.

Tests of the coagulation system include platelet count, prothrombin time (PT), partial thromboplastin time (PTT), fibrinogen, and the thromboelastogram (TEG). Platelet counts, platelet function, PT, and PTT should all be normal before surgery. Platelet function tests are used in special cases where abnormal platelet function is suspected, and they can be useful in timing surgery as they reveal when the antiplatelet effects of drugs have ended. The PTT and the PT measure multiple coagulation factors predicting coagulation deficits. The TEG has been used since the 1940s and became useful in guiding coagulation therapies in liver and aortic surgeries. TEG data are usually available within 30 minutes of draw time. Information on laboratory testing and terms is available in Box 84.1 .

Box 84.1

Laboratory Tests for Hemostasis in Surgery

Prothrombin test (PT) measures coagulation factors VII, X, V, II, and I.
Partial thromboplastin time (PTT) measures coagulation factors XII, XI, IX, VIII, X, V, II, and I.
Platelet count measures the number of platelets in blood. Low levels suggest impaired function. Platelet count for spine surgery should be in the normal range listed for the specific lab where the test was completed. Typical counts for spine surgery should range from 150,000 to 400,000.
Platelet function tests evaluate platelet function. Acquired platelet dysfunction from drugs can be monitored to assure normal platelet function before surgery.
Complete blood count measures hemoglobin, hematocrit, and platelet count, as well as several other indices.
Fibrinogen, factor I in the clotting cascade, is converted to fibrin by thrombin. Low fibrinogen levels are indicative of disseminated intravascular coagulation (DIC).
d -dimer indicates clot lysis and will be markedly elevated in cases of DIC.
Thromboelastogram (TEG) evaluates the entire clot formation process from activation of platelets to clot formation, contraction, and fibrinolysis. It yields multiple data values. The r value, measured in minutes, reflects the reaction time delay from the initiation of the clotting process until the production of fibrin. The r value corresponds to the PT and PTT. Kinetic time (k) measures the time from initial fibrin formation to a specific amount of clot stiffness. This is the time in minutes from fibrin appearance at 2-mm thickness until a thickness of 20 mm has been achieved. The rate of fibrin formation is reflected in the alpha angle (alpha). This is measured by drawing a tangent from the zero axis on the graph measuring the r time and is a function of platelet count and fibrin levels because this angle reflects the interaction of activated platelets and fibrin as they form clots with a larger angle, representing faster clot formation. Maximum amplitude refers to the maximum amount of clot formation and is a measurement of clot strength. Maximum angle mirrors platelet count and fibrin concentration, so as in all types of materials thicker is stronger. Fibrinolysis is assessed with a value called lysis-30, which is the amount of clot that has dissolved within 30 minutes of reaching the maximum amplitude. Lysis-30 will reveal if fibrinolysis is occurring at an abnormally rapid rate. Recommendations for component replacement based on TEG values are as follows: for an r time of greater than 15 minutes infuse two units of fresh frozen plasma, for a maximum amplitude of less than 40 mm infuse 10 units of platelets, and for an alpha angle of less than 40 degrees infuse six units of cryoprecipitate. TEG can guide antifibrinolytic therapy, as Amicar or tranexamic acid will be of benefit in cases of hyperfibrinolysis. [Gastroenterol Hepatol. 2012: 8(8):1-12.]
Metabolic panel measures serum chemistries and renal function with the blood urea nitrogen and creatinine. Liver enzymes may also be assessed, indicating abnormal liver function in some cases. Liver dysfunction and renal failure will affect clotting and hemostasis.

Medication History

Patients with a history of transient ischemic attack, stroke, deep venous thrombosis (DVT), vascular stents, heavy bleeding after minor trauma, alcoholism, hepatic dysfunction, neuromuscular scoliosis, cerebral palsy, and cardiac disease have an increased risk of bleeding, either from the disease state or from pharmacological therapies for their condition.

Patients who take warfarin (Coumadin) may require cessation or acute reversal of anticoagulation. Occasionally, under the guidance of their internist, cardiologist, or hematologist, bridge therapy may be recommended. Patients will be placed on a shorter-acting anticoagulant or antiplatelet agent (commonly subcutaneous injection of low molecular weight heparin) to provide protection during the period of time in which their usual anticoagulant drug therapy is suspended. Bridge therapy substitutes a shorter-acting anticoagulant for one with a longer half-life and thereby lessens risk of vascular misadventure. The shorter-acting agent is suspended shortly before surgery to allow for safe spine surgical intervention, while also minimizing the risk of a thrombotic event. Those rare patients with congenital coagulation deficits typically require consultation with a hematologist and often perioperative selective clotting factor replacement.

Multiple oral anticoagulants called direct-acting oral anticoagulants and antiplatelet drugs are emerging on the marketplace or are now commonly in use. Knowledge of these medications is critical to preoperative planning. Many of these drugs have no known antidote or reversal agent or, where they exist, they can be prohibitively expensive. Platelet function can be impaired by drugs including aspirin (acetylsalicylic acid [ASA]), nonsteroidal antiinflammatory drugs, and specific platelet inhibitors. ASA can be held preoperatively in most patients without deleterious effects. However, patients with known coronary or cerebral vascular disease or significant risk factors for coronary artery disease should remain on ASA at a dose of 75 to 81 mg to lessen the risk of infarction in the perioperative period. Abrupt ASA cessation may cause a rebound effect on platelet aggregation, increasing risk of arterial thrombosis. In cases where ASA should be continued, surgical bleeding can be expected to be 1.5 times greater than normal, but the overall risk to the patient is lessened.

Nutritional supplements and herbs that inhibit platelet function include alfalfa, anise, bilberry, bladderwrack, bromelin, cat’s claw, celery, soleus, Cordyceps, dong quai, evening primrose oil, fenugreek, feverfew, garlic, ginger, ginkgo biloba, ginseng, grape seed, green tea, guggul, horse chestnut seed, horseradish, licorice, prickly ash, red clover, reishi, same, sweet clover, turmeric, and white willow. In general, all supplements should be held for 2 weeks before surgery because their exact ingredients and their physiological effects are highly variable and not well studied.

Table 84.1 contains a listing of medications that interfere with coagulation, and Table 84.2 lists the protein complex concentrates available today as reversal agents for some anticoagulant drugs. The table lists antidotes where known and gives reported guidelines, estimating the amount of time that must pass before the anticoagulant effects of these medications abate. These estimates are based on the time equivalent to three to four drug half-lives and are more restrictive than those published for needle-based procedures. The primary path for drug metabolism is annotated in the table to alert surgeons treating patients with renal failure/insufficiency or liver dysfunction to agents in which the time needed for coagulation to normalize will be increased. The estimated wait times after drug cessation reported in this table are longer than those noted in other surgical literature because spine surgeries are associated with greater blood loss than most other types of surgeries, and this greater blood loss stresses the coagulation system more than small, less invasive procedures. These timelines are recommendations based on experience and synthesis of the limited literature on the topic, as higher-level evidence guiding the optimal perioperative management of anticoagulation medications is lacking.

Table 84.1

Anticoagulants and Antiplatelets

Drug	Class	Mechanism of Action	Half Life	Antidote	Time to Stop Drug before Surgery	Excretion	Metabolism
Abciximab (Repro)		Glycoprotein Iib/IIIa receptor antagonist	10 minutes	Platelet transfusion	120 hours
Aggrastat (Tirofiban)	Antiplatelet	Reversibly binds to platelet glycoprotein IIb/Iia receptors reducing aggregation	2 hours		8 hours	Urine 65%, feces 25%	Minimal
Aggrenox (Aspirin/Dipyradamole)	Antiplatelet	See aspirin and dipyramole			See individual drugs
Agrylin (Anagrelide)	Antiplatelet	Disrupts megakaryocyte development reducing platelet count	1.3 hours		Used for thrombocythemia, adjust dose to keep platelet counts below 600,000	Urine	Liver
Angiomax (Bibalirudin)	Anticoagulant	Reversibly inhibits thrombin	25 minutes	None	1 hour	Urine	Plasma
Argatroban	Anticoagulant	Direct thrombin inhibitor	51 minutes	None	2 hours	Feces 65%, urine 22%	Liver
Arixtra (Fondaparinux)	Anticoagulant	Selective factor Xa inhibitor	21 hours	PCC, rFVIIa	Recommended 24 hours before CABG, 4 days for spinal surgery	Urine	Unknown
Aspirin (Bayer Aspirin, Bayer Low Dose Aspirin, Bayer Low Dose Women’s Aspirin, Bufferin, Ecotrin, Ecotrin Low Strength, St Joseph, St Joseph Regular Strength)	Antiplatelet, Salicylate	Nonselectively and irreversibly inhibits cyclooxygenase. Irreversibly inhibits platelet for its lifespan	6 hours		14 days	Urine	Liver
Atryn (Antithrombin)	Anticoagulant	Inhibits thrombin and factor Xa neutralizes coagulant effects	17 Hours	None	72 hours	Other	Unknown
Betrixaban (Bevyzza)	Anticoagulant	Direct factor Xa inhibitor	24 hours	Andexanet alfa	4 days	Feces
Brilinta (Ticagrelor)	Antiplatelet	Reversibly binds, reducing platelet activation and aggregation	9 hours		7 days	Bile	Liver
Cangrelor (Kengreal)	Antiplatelet		3 minutes	Drug cessation
Celecoxib (Celebrex)	NSAID	Inhibits cyclooxygenase-2	11 hours		5 days	Feces 57%, urine 27%	Liver
Cilostazol (Pletal)	Antiplatelet	Reduces platelet aggregation, reversible	13 hours		5 days	Urine 74%, feces 20%	Liver
Clopidogrel (Plavix)	Antiplatelet	Irreversibly binds to P2Y12 adenosine diphosphate receptors, inhibiting platelet for its lifetime	8 hours		24 days	Urine 50%, feces 46%	Liver
Coumadin (Warfarin, Jantoven)	Anticoagulant	Inhibits vitamin K–dependent factors II, VII, IX, X, protein C, protein S	Variable 20–60 hours	FFP, vitamin K, PCC	120 hours	Urine	Liver
Danaparoid (Orgaran, Organon)	Anticoagulant	Inhibits factors Xa, IIa	24 hours	rFVIIa 90 mcg/kg IV	2 days	Renal
Diclofenac (Arthrotec, Cambia, Cataflam, Flector, Pennsaid, Voltaren, Zipsor, Zorvolex)	NSAID	Inhibits cyclooxygenase	2 hours		5 days	Urine 65%, bile 35%	Liver
Diflunisal (Dolobid)	Salicylate	Inhibits prostaglandin synthesis (reversible)	12 hours		2 days	Urine
Dipyridamole (Persantine)	Antiplatelet	Inhibits platelet adenosine uptake reducing aggregation	10 hours		2 days	Bile	Liver
Edoxaban (Savaysa)	Anticoagulant	Factor Xa inhibitor	10–14 hours	Andexanet alfa	2 days	Urine 50%
Effient (Prasugrel)	Antiplatelet	Irreversibly binds to P2Y12 adenosine diphosphate receptors inhibiting platelet for its lifetime.	7 hours	Drug cessation, platelet transfusion	28 hours	Urine 68%, feces 27%	Liver
Eliquis (Apixaban)	Anticoagulant	Factor Xa inhibitor	12 hours	Andexxa- factor Xa recombinant 400 mg or 800 mg IV bolus. Future (once approved): Ciraparantag	36 hours	Urine 27%, feces	Liver
Enoxaparin (Lovenox)	Anticoagulant	Binds to antithrombin III inhibiting factor X and Xa	7 hours	Protamine 1 mg IV for each mg of Enoxaparin given. Future (once approved): Ciraparantag	24 hours	Urine 40%	Liver
Eptifibatide (Integrlin)		Glycoprotein Iib/IIIa receptor antagonist	3 hours	Drug cessation, platelet transfusion		Renal
Etodolac (Lodine)	NSAID	Reversibly inhibits cyclooxygenase 1 and 2	8 hours		5 days	Urine 73%
Fenoprofen (Naflon)	NSAID	Inhibits cyclooxygenase	3 hours		5 days	Urine 90%	Liver
Flurbiprofen (Ansaid)	NSAID	Inhibits cyclooxygenase	8 hours		5 days	Urine 70%, feces 30%
Fondaparinux	Anticoagulant	Binds to antithrombin III inhibiting factor X and Xa	21 hours	None	96 hours	Urine	Unknown
Fondaparinux (Arixtra)	Pentasaccharide anticoagulant	Selective factor Xa inhibitor	21 Hours	PCC, rFVIIa	2 days
Fragmin (Dalteparin)	Anticoagulant	Binds to antithrombin III, inhibiting factors X and Xa	5 hours	Protamine 1 mg IV for each mg of heparin given. Future (once approved): Ciraparantag, rVIIa.	24 hours	Urine	Liver
Heparin	Anticoagulant	Binds to antithrombin III, inactivates X	1.5 hours	Protamine 1 mg IV for each mg of heparin given. Future (once approved): Ciraparantag, rVIIa.	6 hours	Urine	Liver
Ibuprofen (Advil, Motrin, Caldolor, Duexis)	NSAID	Reversibly inhibits cyclooxygenase	2 hours		5 days	Urine	Liver
Idraparinux	Pentasaccharide anticoagulant	Factor Xa inhibitor	80 hours	PCC, rFVIIa
Indomethicin (Indocin)	NSAID	Inhibits cyclooxygenase	12 hours		5 days	Urine 60%, feces/bile 33%	Liver
Inohep (Tinzaprin)	Anticoagulant	Unknown		None	Unknown	Urine	Unknown
Integrilin (Eptifibatide)	Antiplatelet	Reversibly binds to platelet glycoprotein IIb/IIIa receptors, reducing platelet aggregation	2.5 hours		5 hours	Urine 50%	Minimal
Ipravisk (Desirudin)	Anticoagulant	Direct thrombin inhibitor	2 hours	None	6 hours	Urine	Kidney
Ketoprofen	NSAID	Inhibits cyclooxygenase	2 hours		5 days	Urine 90%	Liver
Ketorolac (Sprix, Toradol)	NSAID	Reversibly inhibits cyclooxygenase 1 and 2	2 to 19 hours		5 days	Urine 92%
Meclofenamate	NSAID	Inhibits cyclooxygenase	1.3 hours		5 days	Urine 70%, feces 30%	Liver
Mefenamic acid (Ponstel)	NSAID	Inhibits cyclooxygenase	2 hours		5 days	Urine 52%, feces 20%	Liver
Meloxicam (Mobic)	NSAID	Inhibits cyclooxygenase	20 hours		5 days	Urine, feces	Liver
Nabumetone (Relafen)	NSAID	Reversibly inhibits cyclooxygenase 1 and 2	24 hours		5 days	Urine 80%
Naproxen (Aleve, Anaprox, Naprosyn, Vimovo, Treximet)	NSAID	Inhibits cyclooxygenase	17 hours		5 days	Urine	Liver
Oxaprozin (Daypro)	NSAID	Inhibits cyclooxygenase	22 hours		5 days	Urine 65%, feces 35%	Liver
Piroxicam (Feldene)	NSAID	Inhibits cyclooxygenase	50 hours		14 days	Urine, feces	Liver
Pradaxa (Dabigatran)	Anticoagulant	Directly reversibly inhibits thrombin	17 hours	Praxbind (Idarucizamab) 5 g × 1, future (once approved): Ciraparantag	72 hours	Urine	Liver
Refludan (Lepirudin)	Anticoagulant	Unknown/drug not available in United States		None	Unknown	Unknown	Unknown
Reopro (Abciximab)	Antiplatelet	Binds to platelet glycoprotein IIb/IIIa receptors, reducing platelet aggregation	10 minutes		1 hour	Urine	Unknown
Salsalate	Salicylate	Inhibits prostaglandin synthesis	16 hours		5 days	Urine	Liver
Sulindac (Clinoril)	NSAID	Inhibits cyclooxygenase	16 hours		5 days	Urine 50%, feces 25%	Liver
Thrombate III (Antithrombin III)	Anticoagulant	Forms covalent bond with thrombin/only for use in congenital ATIII deficiency	3 days	None	Hematology consult needed	Other	Unknown
Ticagrelor (Brilinta)	Antiplatelet	Reversibly binds to ADP receptors	9 hours	PB2452 pending FDA approval	2 days	Feces
Ticlid (Ticlopidine)	Antiplatelet	Irreversibly binds to P2Y12 adenosine diphosphate receptors, reducing platelet aggregation	5 days if repeated dosing		29 days	Urine 60%, feces 23%	Liver
Tinzaprin (Innohep)	Anticoagulant			Protamine 1 mg IV for each mg of heparin given. Future (once approved): Ciraparantag, rVIIa
Tirofiban (Aggrastat)		Glycoprotein Iib/IIIa receptor antagonist	2 hours	Platelet transfusion
Tolmetin	NSAID	Inhibits cyclooxegenase	5 hours		5 days	Urine	Liver
Valproic acid (Depakene)	Antiepileptic	Inhibits platelet function	16 hours		72 hours
Vorapaxar (Zontivity)	Antiplatelet	Inhibits PAR-1	13 days	No antidote	52 days	Feces
Xarelto (Rivaroxaban)	Anticoagulant	Factor Xa inhibitor	9 hours	Andexxa- Factor Xa recombinant 400 mg or 800 mg IV bolus. Future (once approved): Ciraparantag	36 hours	Urine 66% feces 28%	Liver

PCC, Protein complex concentrates; CABG , coronary artery bypass graft; NSAID , nonsteroidal antiinflammatory drug; FFP , fresh-frozen plasma; IV, intravenous; ATIII , antithrombin III; ADP , adenosine diphosphate; FDA , U.S. Food and Drug Administration.

Table 84.2

Protein Complex Concentrates Antidotes

Name	Type	Factor II	Factor VII	Factor IX	Factor X	Protein C	Protein S	Protein Z	Antithrombin III	Heparin	Emergent Dose
Bebulin	3 Factor PCC	100	<5	100	100						50–60 IU/kg IV
Preconativ	3 Factor PCC	83.3		100	83.3						Dose (IU) = body weight (kg) × desired factor IX increase (% of normal or IU/dL)
Proplex-T	3 Factor PCC	50	400	100	50						1.0 unit/kg × body weight (in kg) × desired increase (% of normal
Prothrombinex-HT	3 Factor PCC	100	Low	100	100						(25–50 units/kg
Profilnine SD	3 Factor PCC	150	35	100	100						1.0 unit/kg × body weight (in kg) × desired increase (% of normal
Beriplex (Kcentra)	4 Factor PCC	106.9	55	100	141.4	120.7	86.2	124.1	2.1	1.7	Pharmacy calculation based on weight and INR not to exceed 5000 units
Cofact	4 Factor PCC	56–140	28–80	100	56–140						Pharmacy calculation based on weight and INR not to exceed 5000 units
Kaskadil	4 Factor PCC	148	40	100	160					20	Not available in United States
Octaplex	4 Factor PCC	50–129	50–129	100	50–129	50–129	50–129			20–48	Pharmacy calculation based on weight and INR not to exceed 5000 units

PCC , Protein complex concentrates; IV , intravenous; IU , international units; INR , international normalized ratio.

Preoperative Estimation of Blood Loss

Factors increasing blood loss during spine surgery include tumor, preoperative anemia, increased numbers of levels fused, pulmonary disease, patient habitus and positioning, anticoagulants, and antiplatelet drugs. ^, ^, When surgery is contemplated for reconstruction in cases of spinal metastasis from renal cell carcinoma, preoperative embolization has been shown to significantly reduce intraoperative blood loss. Further, embolization should be considered as a preoperative adjunct in all vascular spinal tumors to minimize blood loss.

Blood loss for any operation should be estimated and plans generated to ensure that blood can be replaced if needed. An estimate of 200 mL of blood lost per fused segment can be made preoperatively to plan if and how much blood will be required for replacement. Patients can usually tolerate a loss of 15% of the blood volume before transfusion. In a 70-kg patient, estimating 70 mL blood/kg body weight, a volume of 735 mL would reflect a 15% blood loss. Table 84.3 outlines the calculations used to determine percentage blood loss and amount of blood loss required to reach a specified Hgb level. Where blood loss is greater, transfusion thresholds have shifted to be more restrictive over time. The volume of blood lost or preplanned Hgb transfusion trigger should be calculated before the start of the procedure and communicated to the anesthesia provider. Although higher (“liberal”) trigger points (Hgb 9–10 g/dL) have been used historically, more recent study demonstrates that lower thresholds provide better outcomes, especially in healthy patients. Recent guidelines published in 2016 by the AABB (formerly the American Association of Blood Banks) and the Journal of the American Medical Association recommend a restrictive red blood cell (RBC) transfusion policy, with transfusion recommended for patients undergoing orthopedic procedures who have a Hgb of 8 g/dL in the postoperative period. A Hgb as low as 7 g/dL can be used as a transfusion trigger for healthy patients undergoing surgical procedures who are no longer bleeding acutely, whereas unhealthy patients with known coronary artery disease or cancer may require a higher threshold (Hgb >9 g/dL) ( Box 84.2 ).

Table 84.3

Calculation of Blood Loss

From American College of Surgeons. ATLS Student Course Manual, 10th ed. Chicago: ACS; 2018.

Parameter	Class I	Class II (Mild)	Class III (Moderate)	Class IV (Severe)
Approximate blood loss	<15%	15%‒30%	31%‒40%	>40%
Heart rate	↔	↔/↑	↑	↑/↑↑
Blood pressure	↔	↔	↔/↓	↓
Pulse pressure	↔	↓	↓	↓
Respiratory rate	↔	↔	↔/↑	↑
Urine output	↔	↔	↓	↓↓
Glasgow Coma Scale score	↔	↔	↓	↓
Base deficit ^a	0 to ‒2 mEq/L	‒2 to ‒6 mEq/L	‒6 to ‒10 mEq/L	‒10 mEq/L or less
Need for blood products	Monitor	Possible	Yes	Massive transfusion protocol

a Base excess is the quality of base (HCO _3– , in mEq/L) that is above or below the normal range in the body. A negative number is called a base deficit and indicates metabolic acidosis.

Box 84.2

Useful Hemostatic Recipes

1.
Cherry solution of liquid clotter: one jar of Codman Spongostan mixed with 8 mL of thrombin containing 1000 units of thrombin per mL of saline. Mix together in a 20-mL syringe with a 12-G Angiocath as a directional nozzle. Apply directly to bleeding tissue.
2.
Fibrin glue: two syringes. First syringe contains fresh-frozen plasma; second syringe contains 1 ampule of calcium chloride and thrombin 10,000 to 20,000 units, and can contain antibiotics. Inject the contents of the syringes simultaneously to form fibrin glue.
3.
FloSeal: commercial product.

Autologous Blood Use

Autologous blood donation, although previously a more common strategy, has lost favor in recent years, especially preoperative donation, as it does not appear to significantly reduce the need for allogenic transfusion. A review of the National Inpatient Sample database (2004‒2009) demonstrated that preoperative autologous donation was actually a significant predictor of allogenic transfusion after spine surgery, especially following fusion of the thoracolumbar spine. That said, in certain patients where the estimated blood loss exceeds 15% to 30% of the blood volume, autologous blood donation remains an option in the perioperative blood management program.

Autologous blood can be obtained in three ways: preoperative donation, intraoperative salvage, and postoperative salvage. The benefits (in terms of decreased allogenic transfusion rates) of salvage techniques are greater, and the costs and risks are lower than preoperative donation, thus they are still commonly used, especially in cases in which higher blood loss is predicted, like posterior deformity surgery. Although preoperative donation is expensive, a reduction in the potential for allogenic transfusion-related morbidities, like transfusion reaction and infection transmission, may offset the cost. Nevertheless, there are risks to autologous blood transfusions, which include septicemia from bacterial contamination of the unit, nonimmune hemolytic transfusion reactions (HTRs), febrile reactions, and volume overload, with the most common still being clerical error.

One unit of blood can be predonated per week if the hematocrit (Hct) remains above 34%. Other guidelines for autologous donation include a patient age range of 12 to 70 years and a Hgb of at least 11 mg/dL. Full units can be taken from patients weighing more than 50 kg, and half units from those between 25 and 50 kg. Supplemental iron is recommended. In some instances, recombinant erythropoietin can be administered to facilitate increased blood volume for autologous donation. ^, This has been shown to increase blood production significantly in both animal and clinical studies.

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