Introduction
A transfusion is defined as an infusion of whole blood or any one of its components. Transfusions, like any other medical intervention, have benefits and risks, and one risk is a hemolytic transfusion reaction (HTR). Hemolysis is the rupture and subsequent leakage of red blood cells (RBCs) into intravascular (in the circulation) or extravascular (in the reticuloendothelial system) spaces. HTRs can also be immune-medicated or non–immune-mediated.[1][2][3]
Immune HTRs often occur due to mismatch or incompatibility of the patient with the donor products and are classified as acute versus delayed hemolytic reactions. Acute hemolytic reactions occur within 24 hours of transfusion, and delayed hemolytic reactions are seen after 24 hours. Delayed reactions usually present 2 weeks after transfusion but can occur up to 30 days post-transfusion. The severity of the hemolytic reaction is dependent on the type and quantity of antigens, alloantibodies, and the presence or absence of complement system activation.
Non-immune hemolysis can be due to thermal, osmotic, or mechanical injury to blood products. Human or systemic errors can cause these forms of hemolysis. HTRs occur most often after the transfusion of packed RBCs but can also occur after the transfusion of other blood products such as plasma, platelets, cryoprecipitate, or whole blood.[4][5]
Etiology
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Etiology
Transfusion of blood components is among the most common procedures for inpatients and outpatients. In the US, an estimated 12.5% of inpatient encounters involve transfusion of blood products. This breakdown results in the transfusion of RBCs in about 11% of encounters and the transfusion of platelets or plasma in about 3%; the total sum is >12.5% because some patients had both.[6]
The incidence of transfusion reactions varies significantly by institution due to differing reporting requirements but is estimated to occur in approximately 0.1% to 3% of all transfusion encounters.[6][7][8] The most common types of transfusion reactions include fever and non-severe allergic reactions, with manifestations such as rash, urticaria, and pruritus. These reactions collectively account for approximately 70% to 80% of all transfusion-related adverse events.[6][8] About 7% of all reactions can be classified as severe, with symptoms such as respiratory distress, hypotension, decreased consciousness, or hemoglobinuria.[8]
The median time for severe reactions was 20 minutes, while the median time for non-severe reactions was significantly longer at 100 minutes. This data suggests that monitoring patients closely for 2 hours after transfusions will likely detect most transfusion reactions; patients should be monitored for at least one hour for severe reactions.[8]
Hemolytic reactions are uncommon, with the incidence reported as 1% to 3% of total transfusion reactions.[6][8] The causes of HTRs can be preventable (human or systemic error) or unavoidable, such as unidentified immune incompatibility. HTRs are classified as immune-mediated or non–immune-mediated. Immune reactions are further divided into acute and delayed reactions. In addition, hemolysis is classified into intravascular and extravascular.[9][10]
Patients with a history of prior transfusion reactions or multiple past transfusions are at a higher risk of experiencing more severe transfusion reactions, possibly due to alloimmunization. The use of preventative measures and washed blood products may be warranted in these patients.[8]
Epidemiology
The prevalence of acute HTRs has been estimated at approximately 1 in 70,000 blood products transfused. The incidence of delayed HTRs remains uncertain due to underreporting, as most patients are asymptomatic. Estimates for this type of reaction vary, ranging from 1 in 800 transfusions to 1 in 11,000 transfusions. The incidence of non–immune hemolytic reactions is also unknown; however, it is also thought to be very rare. Many systems have been implemented to reduce the incidence of HTRs due to human and systemic errors.[11]
Pathophysiology
The different types of hemolytic reactions depend on the etiology. Intravascular hemolysis occurs when an antibody causing complement activation binds an RBC antigen. Extravascular hemolysis occurs when an antibody targeting an RBC antigen opsonizes the RBC, which leads to sequestration and phagocytosis by macrophages, dendritic cells, and neutrophils of the reticuloendothelial system, with primary involvement in the liver, spleen, and bone marrow. Macrophage activation also increases the production of proinflammatory cytokines that induce a systemic response, resulting in symptoms such as fever, chills, abdominal flank pain, and back pain.
For acute hemolytic reactions, the usual incompatibility is blood group system ABO. However, there can also be reactions with other "minor" antigens such as Duffy and Kell. Acute HTRs are most common with transfusion of RBCs but can occur with any blood product. Individuals tend to produce antibodies against antigens absent on their RBC surfaces. This phenomenon is a fundamental principle in blood bank cross-matching procedures. For example, patients with blood group O make antibodies to A and B, while patients with blood type A make antibodies to B and vice versa. Historically, type O blood has been considered a "universal donor" type; however, recent studies have demonstrated the presence of anti-A and anti-B antibodies even without known prior donor exposure. These antibodies are exceptionally high in blood donations from females younger than 40, raising the possibility of additional testing for these donors.
A potential mechanism for ABO incompatibility involves exposure to intestinal microorganisms that possess structures resembling the A and B antigens. This exposure can trigger the production of cross-reactive antibodies with the genuine A and B antigens when encountered. This phenomenon is referred to as molecular mimicry. In the case of other antigens, patients typically need prior exposure to the antigen, which can occur during pregnancy, blood transfusion, or needlestick injuries.
Delayed transfusion reactions often result from an amnestic response, a secondary immune reaction of the immune system to a foreign RBC antigen previously encountered. This prior exposure can occur through events such as pregnancy or previous blood transfusions. The antibody may be so weak as to escape detection on initial cross-match, but the subsequent exposure to the antigen can trigger new antibody formation. Hemolysis is mostly extravascular, of slower and longer duration, and the symptoms are less pronounced compared to an acute hemolytic reaction. The implicated antigens are usually minor antigens like Rh, Kidd, Duffy, Kell, and the MNS constituents.[11]
Thermal, osmotic, and mechanical injury are the most common non-immune reactions. Thermal injury is divided into excess heat or freezing. Excessive heat damages the RBC membrane, causing spontaneous RBC lysis, known as intravascular hemolysis. The blood cells that are not lysed are cleared from the circulation by the spleen through extravascular hemolysis. Freezing injury occurs when RBCs are exposed to below-freezing temperatures in the absence of a cryoprotective agent such as glycerol. This can lead to dehydration injury if the freezing is slow or ice crystal formation if the freezing is rapid, resulting in intravascular hemolysis.
In osmotic injury, hypoosmolar solutions, eg, 5% dextrose, permit free water to enter the RBCs, causing them to swell and lyse (intravascular hemolysis). Mechanical injury is an external force on the RBC causing lysis, known as intravascular hemolysis. This occurs during hemodialysis when RBCs are exposed to physical trauma, such as a small gauge intravenous access or excess transmembrane pressure. Of note, there is an obligate amount of mechanical RBC hemolysis in the centrifuge techniques most commonly used to separate the different blood components. RBC lysis and further cell breakdown during storage contribute to the diminished shelf-life of RBCs and the need for precautions in special populations such as neonates, infants, and patients at risk for transfusion reactions.[12]
When recipient antibodies target and attack donor RBCs, this is referred to as "major incompatibility."Conversely, when donor antibodies attack recipient RBCs, it is termed "minor incompatibility" because fewer antibodies are involved. Inter-donor incompatibility is a very rare condition in which antibodies in donor plasma interact with antigens on the erythrocytes of another donor from a prior transfusion.[11]
Another potential HTR is the sickle cell hemolytic reaction syndrome, characterized by a delayed HRT in patients with sickle cell disease who have developed autoantibodies as a result of previous transfusions. Due to cross-reactivity, there is hemolysis of the donor RBCs, and there can also be hemolysis of the patient's own RBCs.[11] Patients have pain symptoms or dark urine days to weeks after the RBC transfusion; these symptoms can sometimes be misdiagnosed as veno-occlusive disease.[13]
Passenger lymphocyte syndrome occurs when donor lymphocytes, whether solid organ or bone marrow, are transmitted with the transplant. They produce antibodies, especially those towards minor incompatibility targets on the recipient's erythrocytes, causing hemolysis; this is delayed in onset and presents as anemia and jaundice.[14][15] These findings occur immediately posttransplant and can obscure other transplant issues.
Histopathology
In HRTs, a peripheral blood smear will often reveal evidence of hemolysis, which may include the presence of keratocytes, helmet cells, bite cells, blister cells, spherocytes, or microspherocytes. These abnormal RBC shapes and forms are indicative of the destruction of RBCs that can occur in such reactions.
History and Physical
Classically, an acute HTR is described as a triad of symptoms: fever, flank pain, and red or brown urine (hemoglobinuria).[16] However, this classic presentation is rarely seen. Symptom onset is within 24 hours of the transfusion, usually within the first hour. Symptoms may include agitation, chills, burning at the infusion site, chest pain or tightness, headache, nausea, vomiting, and dyspnea. Signs, such as fever, flushing or edema of the skin, tachycardia, hypotension, and reddish-colored urine, may be observed. Diffuse bleeding due to disseminated intravascular coagulation (DIC) or decreased urine output due to renal failure are later signs.
Delayed transfusion reactions can be similar to acute HRTs but more insidious, and presentation is 24 hours to 30 days posttransfusion. Presenting symptoms are most often fever, jaundice, and signs of anemia. Mortality is rare with delayed HRTs, but morbidity increases and hospital stays can be prolonged.
Acute HTR symptoms often are not specific [1][2] and can include agitation; chills; burning sensation at the infusion site; chest, abdomen, or back pain; headache; nausea; vomiting; tachypnea; and dyspnea. Signs such as fever, skin changes (eg flushing, edema, or paleness), tachycardia, hypotension, or urine color change (transparent reddish color) can be seen. Diffuse bleeding may follow as a sign of DIC or anuria due to renal failure. Especially in an anesthetized patient with missing subjective signs, shock, hemoglobinuria, and systemic hemorrhagic state may be the first symptoms of an acute HTR.
Delayed HTR symptoms may be similar to those of an acute HTR but are often less severe. Malaise, fever of unknown origin, and clinical signs of anemia may be present. An unexplained fall in hemoglobin and mild jaundice about one week after blood transfusion can be symptoms of delayed HTR. Sometimes, hemoglobinuria is seen in a delayed HTR, but renal failure is uncommon. Death caused by a delayed HTR is very rare, but in critically ill patients, delayed HTR may add to other severe conditions. In several cases, however, a delayed HTR after incompatible RBC transfusion shows no clinical symptoms but is only recognized—often by chance—by laboratory investigations like positive antibody tests. In such cases, referring to this as a delayed serological transfusion reaction might be more appropriate, as it involves serological (immune-mediated) mechanisms and occurs after some time following the transfusion.[19][20]
Evaluation
If an acute transfusion reaction is suspected, the transfusion should be stopped, and the blood should be sent back to the blood lab for additional testing. This may also require retesting of the patient receiving the transfusion. The most important tests to look for in immune-mediated hemolysis are direct and indirect Coombs tests, also called direct and indirect antibody tests. Free hemoglobin from the transfusion bag should be measured to evaluate for hemolysis within the transfusion sample, which will cause similar symptoms. Blood cultures from the patient and transfusion sample should be drawn to assess for infection and sepsis.
In delayed transfusion reactions, antibodies should be retested in the patient sample and compared with the patient's pretransfusion sample to evaluate for new autoantibodies. This is important to avoid future occurrences of acute HTRs. Institutions have different protocols for how long samples are kept, which can affect the pretransfusion sample's availability.
Other serum lab tests should be performed, including CBC with peripheral smear, indirect bilirubin, haptoglobin, and lactate dehydrogenase. Urine hemoglobin should also be sent. A basic metabolic panel (BMP) to evaluate renal function and coagulation studies to monitor for DIC should also be sent.[11]
Treatment / Management
HTRs can vary in severity, from mild to severe, and it is crucial to identify and treat them promptly, as they can be life-threatening. The first step is always to stop the transfusion. If clinical suspicion is high or symptoms are severe, such as hypotension, respiratory difficulty, or airway closing, immediate resuscitation and emergency treatment are warranted. Corticosteroids, antihistamines, and epinephrine in the case of airway compromise are usually administered. The patient should be aggressively hydrated unless volume overload is suspected to reduce the complications of free hemoglobin in the bloodstream, such as acute kidney injury or disseminated intravascular coagulation. Exchange transfusion is used as a treatment of last resort.[11]
Differential Diagnosis
The differential diagnosis for acute HRTs is broad and includes non-immune and non-hemolytic reactions to transfusion, including infection from bacteria in the transfusion sample, hemolysis within the transfusion sample, anaphylaxis to components of the transfusion or chemicals used in the separation of blood components, or transfusion of expired blood products. Other underlying pathological states that can have similar symptoms include transfusion-related acute lung injury (TRALI), acute urticaria, drug-induced hemolysis, angioedema, pulmonary edema, cold agglutinin disease, DIC, sepsis, paroxysmal nocturnal hemoglobinuria, hereditary erythrocyte defects (eg, sickle-cell disease, G6PDH deficiency), thrombotic thrombocytopenic purpura, and mechanical hemolysis (eg, from heart valves or dialysis).
Prognosis
Acute HTRs can be life-threatening and require immediate identification. Both acute and delayed HTRs warrant the identification of causative antibodies to avoid severe reactions in the future.[17]
Complications
Transfusion reactions can result in secondary complications, primarily due to the presence of autoantibodies, which raise the risk of future reactions, systemic hypotension-related issues, and the potential development of volume overload leading to cardiopulmonary compromise.[18]
Deterrence and Patient Education
Prevention is the best protocol, and close attention should be paid to systemic protocols to prevent transfusion of incorrect blood products. In addition, the blood bank should thoroughly investigate all transfusion reactions, and appropriate antibody testing should be performed. Patients at high risk for transfusion of blood products should be given appropriate prophylactic treatment before transfusion, usually with steroids and an antihistamine. It is also essential to use a restrictive transfusion system with goal Hgb usually around 7.0 mg/dL for most indications and 8 to 10mg/dL for acute MI or cardiac ischemia.[16]
Enhancing Healthcare Team Outcomes
Managing HTRs requires a cohesive and interprofessional healthcare team to provide patient-centered care, enhance outcomes, ensure safety, and optimize team performance. Physicians, nurses, pharmacists, laboratory staff, and transfusion specialists play pivotal roles in this collaborative approach. Blood products often require at least 2 different staff members to verify patient and transfusion products to prevent administration errors. If a reaction does occur, even if not clinically significant, testing for appropriate antibodies can prevent future severe reactions. This requires immediate identification of the reaction and subsequent efficient processing of the transfusion product for processing.
Effective communication among team members is paramount. Physicians and nurses must promptly recognize HTR symptoms, such as fever, hemoglobinuria, and flank pain. Laboratory staff should ensure accurate cross-matching and compatibility checks. Open and clear communication facilitates rapid diagnosis and treatment decisions, preventing errors and ensuring a coordinated response.
Responsibilities within the team are well-defined. Nurses administer blood products while closely monitoring patients for adverse reactions. Physicians diagnose and initiate treatment, which may include managing life-threatening symptoms like hypotension and respiratory distress. Pharmacists ensure appropriate blood product selection and administration.
Ethical considerations guide care decisions. Informed consent is essential, respecting patient autonomy and ensuring beneficence and non-maleficence. Patient preferences are central to decisions, promoting shared decision-making.
Education and training keep the team updated on best practices. Ongoing professional development ensures that healthcare practitioners are equipped to respond effectively to HTRs.
A patient-centered approach places the patient's well-being and preferences at the forefront of all decisions. In managing HTRs, an interprofessional healthcare team ensures a comprehensive response, minimizes complications, and prioritizes patient safety and care quality.
References
De Cloedt L, Savy N, Gauvin F, Taylor S, Lacroix J, Emeriaud G. Transfusion-Associated Circulatory Overload in ICUs: A Scoping Review of Incidence, Risk Factors, and Outcomes. Critical care medicine. 2019 Jun:47(6):849-856. doi: 10.1097/CCM.0000000000003743. Epub [PubMed PMID: 30882480]
Level 2 (mid-level) evidenceMerle NS, Boudhabhay I, Leon J, Fremeaux-Bacchi V, Roumenina LT. Complement activation during intravascular hemolysis: Implication for sickle cell disease and hemolytic transfusion reactions. Transfusion clinique et biologique : journal de la Societe francaise de transfusion sanguine. 2019 May:26(2):116-124. doi: 10.1016/j.tracli.2019.02.008. Epub 2019 Feb 22 [PubMed PMID: 30879901]
Hod EA. Consequences of hemolysis: Pro-inflammatory cytokine response to erythrophagocytosis. Transfusion clinique et biologique : journal de la Societe francaise de transfusion sanguine. 2019 May:26(2):125-127. doi: 10.1016/j.tracli.2019.02.005. Epub 2019 Feb 22 [PubMed PMID: 30862396]
Zaremba R, Brooks A, Thomovsky E. Transfusion Medicine: An Update on Antigens, Antibodies and Serologic Testing in Dogs and Cats. Topics in companion animal medicine. 2019 Mar:34():36-46. doi: 10.1053/j.tcam.2018.12.005. Epub 2018 Dec 31 [PubMed PMID: 30808496]
Level 3 (low-level) evidenceWood EM, Ang AL, Bisht A, Bolton-Maggs PH, Bokhorst AG, Flesland O, Land K, Wiersum-Osselton JC, Schipperus MR, Tiberghien P, Whitaker BI. International haemovigilance: what have we learned and what do we need to do next? Transfusion medicine (Oxford, England). 2019 Aug:29(4):221-230. doi: 10.1111/tme.12582. Epub 2019 Feb 6 [PubMed PMID: 30729612]
Karafin MS, Bruhn R, Westlake M, Sullivan MT, Bialkowski W, Edgren G, Roubinian NH, Hauser RG, Kor DJ, Fleischmann D, Gottschall JL, Murphy EL, Triulzi DJ, National Heart, Lung, and Blood Institute Recipient Epidemiology and Donor Evaluation Study-III (REDS-III). Demographic and epidemiologic characterization of transfusion recipients from four US regions: evidence from the REDS-III recipient database. Transfusion. 2017 Dec:57(12):2903-2913. doi: 10.1111/trf.14370. Epub 2017 Oct 24 [PubMed PMID: 29067705]
Nitsche E, Dreßler J, Henschler R. Systematic Workup of Transfusion Reactions Reveals Passive Co-Reporting of Handling Errors. Journal of blood medicine. 2023:14():435-443. doi: 10.2147/JBM.S411188. Epub 2023 Aug 8 [PubMed PMID: 37576590]
Level 1 (high-level) evidenceHatayama Y, Matsumoto S, Hamada E, Kojima N, Hara A, Hino N, Motokura T. Analysis of Acute Transfusion Reactions and Their Occurrence Times. Yonago acta medica. 2018 Mar:61(1):87-90 [PubMed PMID: 29599628]
Roubinian N. TACO and TRALI: biology, risk factors, and prevention strategies. Hematology. American Society of Hematology. Education Program. 2018 Nov 30:2018(1):585-594. doi: 10.1182/asheducation-2018.1.585. Epub 2018 Dec 14 [PubMed PMID: 30570487]
Manduzio P. Transfusion-associated graft-versus-host disease: A concise review. Hematology reports. 2018 Nov 6:10(4):7724. doi: 10.4081/hr.2018.7724. Epub 2018 Nov 6 [PubMed PMID: 30542528]
Strobel E. Hemolytic Transfusion Reactions. Transfusion medicine and hemotherapy : offizielles Organ der Deutschen Gesellschaft fur Transfusionsmedizin und Immunhamatologie. 2008:35(5):346-353 [PubMed PMID: 21512623]
Lu M, Lezzar DL, Vörös E, Shevkoplyas SS. Traditional and emerging technologies for washing and volume reducing blood products. Journal of blood medicine. 2019:10():37-46. doi: 10.2147/JBM.S166316. Epub 2019 Jan 3 [PubMed PMID: 30655711]
Thein SL, Pirenne F, Fasano RM, Habibi A, Bartolucci P, Chonat S, Hendrickson JE, Stowell SR. Hemolytic transfusion reactions in sickle cell disease: underappreciated and potentially fatal. Haematologica. 2020 Mar:105(3):539-544. doi: 10.3324/haematol.2019.224709. Epub 2020 Feb 6 [PubMed PMID: 32029505]
Peck JR, Elkhammas EA, Li F, Stanich PP, Latchana N, Black S, Michaels A. Passenger lymphocyte syndrome: a forgotten cause of postliver transplant jaundice and anemia. Experimental and clinical transplantation : official journal of the Middle East Society for Organ Transplantation. 2015 Apr:13(2):200-2. doi: 10.6002/ect.2013.0239. Epub 2014 Jul 31 [PubMed PMID: 25077954]
Level 3 (low-level) evidenceMoosavi MM, Duncan A, Stowell SR, Roback JD, Sullivan HC. Passenger Lymphocyte Syndrome; a Review of the Diagnosis, Treatment, and Proposed Detection Protocol. Transfusion medicine reviews. 2020 Jul:34(3):178-187. doi: 10.1016/j.tmrv.2020.06.004. Epub 2020 Jul 16 [PubMed PMID: 32826130]
Ackfeld T, Schmutz T, Guechi Y, Le Terrier C. Blood Transfusion Reactions-A Comprehensive Review of the Literature including a Swiss Perspective. Journal of clinical medicine. 2022 May 19:11(10):. doi: 10.3390/jcm11102859. Epub 2022 May 19 [PubMed PMID: 35628985]
Level 3 (low-level) evidenceGuo K, Wang X, Zhang H, Wang M, Song S, Ma S. Transfusion Reactions in Pediatric Patients: An Analysis of 5 Years of Hemovigilance Data From a National Center for Children's Health in China. Frontiers in pediatrics. 2021:9():660297. doi: 10.3389/fped.2021.660297. Epub 2021 May 28 [PubMed PMID: 34123967]
Dasararaju R, Marques MB. Adverse effects of transfusion. Cancer control : journal of the Moffitt Cancer Center. 2015 Jan:22(1):16-25 [PubMed PMID: 25504275]