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Human Albumin in Cirrhosis & Liver Failure: Practice Review

Written By : Dr. Kamal Kant Kohli Published On 2026-03-27T10:54:39+05:30  |  Updated On 27 March 2026 11:42 AM IST
Human Albumin in Cirrhosis & Liver Failure: Practice Review
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Chronic liver disease affects 1.5 billion people globally, of whom 18.3% are of Indian origin, indicating a significant liver cirrhosis-related burden in India. Decreased plasma albumin is a major complication in this patient population, with over 75% of decompensated patients having hypoalbuminemia. Albumin administration has shown promise in reducing complications, including infections and renal dysfunction. Beyond volume expansion, albumin exerts pleiotropic effects including antioxidant activity, immunomodulation, and endothelial stabilization. This article explores albumin's potential role in cirrhosis and liver failure as a disease-modifying therapy, not just a supportive fluid.

Albumin in Liver Cirrhosis: Potential Mechanistic Role

Intravenous albumin improves circulatory dysfunction in cirrhosis through dual mechanisms: expanding intravascular volume to enhance cardiac output, while simultaneously increasing systemic vascular resistance via improved albumin function, enhanced antioxidant activity, and decreased nitric oxide synthesis (Figure 1).

Figure 1: Dual Mechanisms of Albumin in Improving Circulatory Dysfunction in Liver Cirrhosis

Albumin in Liver Cirrhosis Outcomes: Review of Clinical Evidence

Albumin on Outcomes in Decompensated Liver Cirrhosis: A meta-analysis of 16 RCTs (n=1,518 cirrhotic patients) evaluated outcomes with and without albumin use. In paracentesis management, albumin significantly reduced the relative risk odds of paracentesis-induced circulatory dysfunction by 74% (R 0.26). Among patients with infections, albumin reduced the relative risk odds of mortality by 54% (OR 0.46), translating to 14% mortality with albumin versus 26% without treatment at three months, and 66% reduction in renal impairment (OR 0.34). In spontaneous bacterial peritonitis specifically, combining albumin with antibiotics reduced in-hospital mortality from 29% to 10%, establishing albumin as an evidence-based intervention for hemodynamic stability and organ preservation in decompensated liver cirrhosis.

Albumin in Overt Hepatic Encephalopathy: Indian Experience: An RCT of 120 Indian cirrhotic patients (70% Child-Pugh Class C) with overt hepatic encephalopathy [HE] (grades 2-4) compared albumin plus lactulose versus lactulose alone. Complete HE reversal was significantly higher with combination therapy (75% vs 53.3%; p=0.03), accompanied by reduced mortality (18.3% vs 31.6%; p=0.04) and shorter hospital stay (6.4±3.4 vs 8.6±4.3 days; p=0.01). Beyond clinical improvement, albumin combination therapy achieved significantly greater reductions in inflammatory cytokines (IL-6: -17.3±4.6 vs -9.4±3.2 pg/mL; IL-18: -33.5±13.4 vs -17.4±11.5 pg/mL; TNF-α: -25.4±7.7 vs -13.7±5.3 pg/mL; all p<0.05) and endotoxin levels (p=0.02), demonstrating albumin's anti-inflammatory and detoxifying mechanisms enhance outcomes in overt hepatic encephalopathy beyond standard ammonia-lowering therapy.

Albumin in Liver Cirrhosis with Ascites: The ANSWER trial, a multicenter randomized study including 431 patients with decompensated cirrhosis and uncomplicated ascites, demonstrated that long-term albumin administration improved 18-month survival compared to standard medical treatment alone (Kaplan-Meier estimates 77% vs 66%; p=0.028), representing a 38% relative reduction in mortality (HR 0.62). Beyond survival benefits, albumin therapy reduced first paracentesis occurrence by 52% (HR 0.48, p<0.0001) with paracentesis incidence rate ratio of 0.46 (95% CI 0.40–0.53), decreased refractory ascites development by 57% (HR 0.43, p<0.0001), and significantly lowered rates of spontaneous bacterial peritonitis (IRR 0.33), hepatorenal syndrome type 1 (IRR 0.39), and severe hepatic encephalopathy (IRR 0.48). Hospital admissions (IRR 0.65) and days spent in hospital (IRR 0.55) were significantly reduced, establishing albumin as disease-modifying therapy in decompensated cirrhosis (Figure 1).

Figure 1. ANSWER Trial: Clinical and Resource Utilization Outcomes. Abbreviations: SMT, standard medical treatment; SBP, spontaneous bacterial peritonitis; HRS, hepatorenal syndrome; HR, hazard ratio.

Real-World Application & Practical Considerations

International consensus and major hepatology societies recommend considering albumin administration in well-defined clinical scenarios with evidence.

Treatment response is best assessed through clinical improvement in hemodynamics, renal function, and ascites control. Routine monitoring helps ensure safe administration, especially with long-term use. 7,8,9,10

Quality Standards & Product Selection

Given cirrhotic patients' immunocompromised state, albumin quality is paramount. Products meeting IQPP and QSEAL standards ensure pathogen safety through rigorous screening and viral inactivation. Hyperoncotic 25% formulations provide greater oncotic effect per volume in fluid-sensitive patients. Closed-system delivery minimizes central line-associated infection risks in vulnerable populations. Product selection should prioritize manufacturing consistency for long-term therapy and practical considerations, including storage stability and contamination prevention during administration.

Key Take-Home Messages

✔ Chronic liver disease affects 1.5 billion people globally with 18.3% of Indian origin, and over 75% of decompensated liver cirrhosis patients have hypoalbuminemia.

✔ Albumin exerts pleiotropic effects including antioxidant activity, endothelial stabilization, and immunomodulation that address systemic inflammation and circulatory dysfunction in decompensated liver cirrhosis.

✔ Clinical evidence demonstrates albumin reduces mortality and complications, with international guidelines recommending albumin for large-volume paracentesis, spontaneous bacterial peritonitis, hepatorenal syndrome, and uncomplicated ascites management.

✔ Albumin products meeting IQPP and QSEAL standards ensure pathogen safety, with hyperoncotic 25% formulations and closed-system delivery minimizing infection risks in immunocompromised cirrhotic populations.

Abbreviations: AGA- American Gastroenterological Association, ACLF - Acute-on-Chronic Liver Failure, AKI - Acute Kidney Injury, APASL - Asian Pacific Association for the Study of the Liver, HE - Hepatic Encephalopathy, HR - Hazard Ratio, HRS - Hepatorenal Syndrome,ICTMG-International Collaboration for Transfusion Medicine Guidelines, IL-6 - Interleukin-6, IL-18 - Interleukin-18, IQPP - International Quality Plasma Program, IRR - Incidence Rate Ratio, LVP - Large-Volume Paracentesis, NO- nitric oxide, OR - Odds Ratio, PVDC - Polyvinylidene Chloride, QSEAL - Quality Standards of Excellence, Assurance, and Leadership, RCT - Randomized Controlled Trial, SBP - Spontaneous Bacterial Peritonitism, SMT - Standard Medical Treatment

References:
  • 1.Swaroop, S., Vaishnav, M., Arora, U., Biswas, S., Aggarwal, A., Sarkar, S., Khanna, P., Elhence, A., Kumar, R., Goel, A., & Shalimar (2024). Etiological Spectrum of Cirrhosis in India: A Systematic Review and Meta-analysis. Journal of clinical and experimental hepatology, 14 -
  • 2.Grüngreiff, K., Gottstein, T., Reinhold, D., & Blindauer, C. A. (2021). Albumin Substitution in Decompensated Liver Cirrhosis: Don't Forget Zinc. Nutrients, 13 -
  • 3.Carvalho, J. R., & Verdelho Machado, M. (2018). New Insights About Albumin and Liver Disease. Annals of hepatology, 17 547-560
  • 4.Arroyo, V., & Fernandez, J. (2011). Pathophysiological basis of albumin use in cirrhosis. Annals of hepatology, 10 Suppl 1, 6-14
  • 5.Kwok, C. S., Krupa, L., Mahtani, A., Kaye, D., Rushbrook, S. M., Phillips, M. G., & Gelson, W. (2013). Albumin reduces paracentesis-induced circulatory dysfunction and reduces death and renal impairment among patients with cirrhosis and infection: a systematic review and meta-analysis. BioMed research international, -
  • 6.Sharma, B. C., Singh, J., Srivastava, S., Sangam, A., Mantri, A. K., Trehanpati, N., & Sarin, S. K. (2017). Randomized controlled trial comparing lactulose plus albumin versus lactulose alone for treatment of hepatic encephalopathy. Journal of gastroenterology and hepatology, 32 1234-1239
  • 7.Caraceni, P., Riggio, O., Angeli, P., Alessandria, C., Neri, S., Foschi, F. G., Levantesi, F., Airoldi, A., Boccia, S., Svegliati-Baroni, G., Fagiuoli, S., Romanelli, R. G., Cozzolongo, R., Di Marco, V., Sangiovanni, V., Morisco, F., Toniutto, P., Tortora, A., De Marco, R., Angelico, M., … ANSWER Study Investigators (2018). Long-term albumin administration in decompensated cirrhosis (ANSWER): an open-label randomised trial. Lancet (London, England), 391 2417-2429
  • 8.Callum, J., Skubas, N. J., Bathla, A., Keshavarz, H., Clark, E. G., Rochwerg, B., Fergusson, D., Arbous, S., Bauer, S. R., China, L., Fung, M., Jug, R., Neill, M., Paine, C., Pavenski, K., Shah, P. S., Robinson, S., Shan, H., Szczepiorkowski, Z. M., Thevenot, T., … International Collaboration for Transfusion Medicine Guidelines Intravenous Albumin Guideline Group (2024). Use of Intravenous Albumin: A Guideline From the International Collaboration for Transfusion Medicine Guidelines. Chest, 166 321-338
  • 9.Garcia-Tsao, G., Abraldes, J. G., Rich, N. E., & Wong, V. W. (2024). AGA Clinical Practice Update on the Use of Vasoactive Drugs and Intravenous Albumin in Cirrhosis: Expert Review. Gastroenterology, 166 202-210
  • 10.Singh V, De A, Mehtani R, et al. Asia-Pacific association for study of liver guidelines on management of ascites in liver disease. Hepatol Int 2023; 792-826
  • 11.Bai, Z., Méndez-Sánchez, N., Romeiro, F. G., Mancuso, A., Philips, C. A., Tacke, F., Basaranoglu, M., Primignani, M., Ibrahim, M., Wong, Y. J., Nery, F. G., Teschke, R., Ferreira, C. N., Muñoz, A. E., Pinyopornpanish, K., Thevenot, T., Singh, S. P., Mohanty, A., Satapathy, S. K., Ridola, L., … Liver Cirrhosis-related Complications (LCC)-International Special Interest Group (2023). Use of albumin infusion for cirrhosis-related complications: An international position statement. JHEP reports : innovation in hepatology, 5 -
human albuminliver cirrhosisliver failurehypoalbuminemiaplasma albumincirculatory dysfunctioninfectionmortalityorgan preservationtransplantsurgeryicuinflammatory cytokinesasciteshospital carehepatorenal syndromebacterial peritonitischronic liver failurebilirubincreatinineseptic shockhyperoncotic
Dr. Kamal Kant Kohli
Dr. Kamal Kant Kohli

Dr Kamal Kant Kohli-MBBS, DTCD- a chest specialist with more than 30 years of practice and a flair for writing clinical articles, Dr Kamal Kant Kohli joined Medical Dialogues as a Chief Editor of Medical News. Besides writing articles, as an editor, he proofreads and verifies all the medical content published on Medical Dialogues including those coming from journals, studies,medical conferences,guidelines etc. Email: drkohli@medicaldialogues.in. Contact no. 011-43720751

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