Urinary trypsin inhibitor: miraculous medicine in many surgical situations?

Jong In Han

doi:10.4097/kjae.2010.58.4.325

Recently, we encounter several articles regarding urinary trypsin inhibitor (UTI) published nationally [1,2]. When we take a glance at these articles, it feels like UTI acts as a miraculous medicine on patients under general anesthesia because of its protection effect against surgical stress. Yet, even after the first report on antitryptic action of urine by Bauer and Reich III in 1909 [3]; the start of use of the term UTI by Astrup and Sterndorff in 1955 [4]; and numerous animal experiments and clinical research done about UTI (803 articles about UTI and 982 articles about ulinastatin in SCOPUS), UTI is not yet to be used commonly. Therefore, it is important to understand the reason behind this situation. According to the webpage of Nextbio, it records that "currently, the drug is being used for research purpose only."

UTI is a glycoprotein stable in both heat and acids derived from human urine, and is a serine protease inhibitor found in human urine or blood. UTI is secreted when inter-α-trypsin inhibitors are degraded by neutrophilic elastase [5]. UTI is found to have many physiologic effects, including the inhibition of neutrophilic elastase, trypsin, α-chymotrypsin, plasmin, and cathepsin G. It has been known for a long time [3] and called ulinastatin, mingin, human inhibitor 30, serpin, miraclid, urinastatin (in japanese literature) and bikunin [6]. It has been reported that, in human, the plasma half-life of UTI is 33 min [7]. Currenlty, there are three pharmaceutical companies in Korea that produce UTI: Ulistin®, Han Lim Pharmaceutical, Ustatin®, Kolon Pharmaceutical, Statin®, Yu Young Pharmaceutical. These three companies produce two types of UTI, which is 50,000 IU (9,962-14,650 won) and 100,000 IU (14,926-21,950 won).

Trypsin inhibitors act to suppress the proteolytic action of trypsin on a variety of tissues and exert a localized anti-inflammatory effect [8]. Therefore UTI is indicated for acute inflammatory disorders, including acute pancreatitis, systemic inflammatory reaction syndrome, circulatory insufficiency, Stevens-Johnson syndrome, Toxic epidermal necrolysis (TEN), disseminated intravascular coagulation (DIC) and multiple organ failure [9]. Previous studies of UTI have focused mainly on modulating inflammatory reaction. UTI attenuates the elevation of neutrophil elastase release, thereby blunting the rise of pro-inflammatory cytokine level; however, the actual mechanism in vivo is not clear [10]. In twenty years, lately, there has been an increase in the number of reports that UTI inhibits secretion of cytokines (IL-6 and IL-8) regarding inflammation. Regardless of such fact, there was an additional report in this issue on how UTI influences cytokine reactions during gastrectomy [1]. This addition of one more report maybe because of the fact that UTI's clinical usage is yet limited and the usage has not been standardized for the real practice. In this issue of KJA, Park and co-workers [1] reported that 100,000 U of UTI infusion during gastrectomy inhibited the secretion of IL-6, which is an inflammatory cytokine produced after operation. They showed that UTI could decrease the inflammatory reaction caused by surgical stress.

In addition to UTI's effect on inflammation, there has been a lot of studies of influence of UTI on shock. In 1985, Ohnishi et al. [11] proved that UTI lowers the elevated enzyme activities in the serum during shock so that UTI has protective effect against shock in his animal experiment. There also has been a study that UTI is effective in maintaining microcirculation during hemodilution and hypothermia [12]. UTI's anti-shock effect was as effective as that of methyl prednisolone (MPS); both substances showed similar effects in endotoxin-induced shock animal experiments [13]. MPS showed effect when after the shock occurred, whereas UTI showed effect when injected prophylactically [14]. Recently, there was a clinical research that the combined usage of UTI and Thymosin alpha1 (Talph1) increased the survival rate of sever sepsis patients [15-17], which proves UTI's usefulness as a potential medicine.

A study about the hemostatic effects of ulinastatin in clinical practice was demonstrated in our journal three months ago [2]. Lee et al. [2] concluded that a single infusion of ulinastatin during major orthopedic surgery reduces blood loss in the early postoperative period. UTI inhibit proinflammatory cytokine release, reduce reperfusion lung injury and preserve pulmonary function but it failed to inhibit platelet activation and to prevent blood loss during CPB [18].

There were studies about UTI's effect on liver, lung, heart, small intestine, pancreas, uterine muscle etc. UTI is important in liver regeneration [19], can protect against sever liver injury [20], and decreases reperfusion injury after hepatic ischemia [21]. High dose of UTI inhibits pulmonary fibrosis by decreasing inflammatory response in lungs [22] and also has protective effect against ischemia/reperfusion injury in lungs. Also, the cardioprotective effect decreases the infarct size in patients with the regional myocardial I/R injury [23]. When UTI is used preventively, pancreatitis occurring frequencies decrease and, through the regulation of intracellular calcium, UTI suppresses the uterine muscle contraction. It furthermore suppresses activity of plasminogen activator, which leads to improvements in joint pain and range of motion in osteoarthritis patients [24].

Saitoh reported contents regarding anesthetic drugs in UTI studies; in neuromuscular junctions, protease inhibitor homologs release acetylcholine which results in delay of onset of neuromuscular block by vecuronium and accelerates the recovery [25]. Mastumoto explained that UTI increases the blood flow in liver [26], so it promotes hepatic elimination of vecuronium and increases urine volume [27]. Because UTI may increase hepatic and/or renal clearance of vecuronium, recovery of vecuronium-induced neuromuscular block would be quickened.

As shown above, UTI will be useful if its various effects are proven clinically and its dose and ways usage are standardized accurately. When used in case of general anesthesia in high-risk patients, UTI can better the microcirculation during circulatory insufficiency which can potentially occur during the operation; therefore, UTI can better the perfusion for main organs and decrease the inflammatory response so that post-surgical progress can be improved, pain be reduced, and mobidity be reduced also. However, UTI's effect on skeletal muscle relaxants used in general anesthesia should be considered. Also due to its comparative high cost, we should avoid reckless and indiscrete usage.

References

1. Park JH, Kwak SH, Jeong CW, Bae HB, Kim SJ. Effect of ulinastatin on cytokine reaction during gastrectomy. Korean J Anesthesiol 2010; 58: 334-337.

2. Lee JY, Lee JY, Chon JY, Moon HS, Hong SJ. The effect of ulinastatin on hemostasis in major orthopedic surgery. Korean J Anesthesiol 2010; 58: 25-30.

3. Bauer J, Reich Z III. Antitryptic action of urine. Med Klin 1909; 5: 1744-1747.

4. Astrup T, Sterndorff I. The plasminogen activator in urine and the urinary trypsin inhibitor. Scand J Clin Lab Invest 1955; 7: 239-245. PMID: 13298600.

5. Hirose J, Ozawa T, Miura T, Isaji M, Nagao Y, Yamashiro K, et al. Human neutrophil elastase degrades inter-alpha-trypsin inhibitor to liberate urinary trypsin inhibitor related proteins. Biol Pharm Bull 1998; 21: 651-656. PMID: 9703243.

6. Pugia MJ, Lott JA. Pathophysiology and diagnostic value of urinary trypsin inhibitors. Clin Chem Lab Med 2005; 43: 1-16. PMID: 15653436.

7. Jonsson-Berling BM, Ohlsson K. Distribution and elimination of intravenously injected urinary trypsin inhibitor. Scand J Clin Lab Invest 1991; 66: 117-122.

8. Fries E, Blom AM. Bikunin-not just a plasma proteinase inhibitor. Int J Biochem Cell Biol 2000; 32: 125-137. PMID: 10687949.

9. Inoue K, Takano H, Yanagisawa R, Yoshikawa T. Protective effects of urinary trypsin inhibitor on systemic inflammatory response induced by lipopolysaccharide. J Clin Biochem Nutr 2008; 43: 139-142. PMID: 19015747.

10. Levi M. Disseminated intravascular coagulation. Crit Care Med 2007; 35: 2191-2195. PMID: 17855836.

11. Ohnishi H, Suzuki K, Niho T, Ito C, Yamaguchi K. Protective effects of urinary trypsin inhibitor in experimental shock. Jpn J Pharmacol 1985; 39: 137-144. PMID: 2418241.

12. Komori M. Effect of ulinastatin on microcirculation under hemodilution and hypothermia. Masui 1990; 39: 741-750. PMID: 2388393.

13. Okano S, Tagawa M, Urakawa N, Ogawa R. A therapeutic effect of ulinastatin on endotoxin-induced shock in dogs-comparison with methylprednisolone. J Vet Med Sci 1994; 56: 645-649. PMID: 7999884.

14. Nakajima K, Goto Y. Differentiation of the anti-shock effect of ulinastatin from steroid hormone by the continuous observation of microcirculation dynamics. Circ Shock 1992; 36: 284-289. PMID: 1623572.

15. Chen H, He MY, Li YM. Treatment of patients with severe sepsis using ulinastatin and thymosin alpha 1: a prospective randomized controlled pilot study. Chin Med J 2009; 122: 883-888. PMID: 19493408.

16. Li Y, Chen H, Li X, Zhou W, He M, Chiriva-Internati M, et al. A new immunomodulatory therapy for severe sepsis: ulinastatin plus thymosin {alpha} 1. J Intensive Care Med 2009; 24: 47-53. PMID: 19033321.

17. Zhang Y, Chen H, Li YM, Zheng SS, Chen YG, Li LJ, et al. Thymosin alpha1-and ulinastatin-based immunomodulatory strategy for sepsis arising from intra-abdominal infection due to carbapenem-resistant bacteria. J Infect Dis 2008; 198: 723-730. PMID: 18613793.

18. Bingyang J, Jinping L, Mingzheng L, Guyan W, Zhengyi F. Effects of urinary protease inhibitor on inflammatory response during on-pump coronary revascularization: effect of ulinastatin on inflammatory response. J Cardiovasc Surg 2007; 48: 497-503. PMID: 17653011.

19. Nobuoka T, Mizuguchi T, Oshima H, Shibata T, Kaji S, Nagayama M, et al. Impaired liver regeneration with humoral and genetic disturbances in urinary trypsin inhibitor-deficient mice. Liver Int 2009; 29: 979-987. PMID: 19302180.

20. Takano H, Inoue K, Shimada A, Sato H, Yanagisawa R, Yoshikawa T. Urinary trypsin inhibitor protects against liver injury and coagulation pathway dysregulation induced by lopopolysaccharide/D-galactosamine in mice. Lab Invest 2009; 89: 833-839. PMID: 19398962.

21. Wu YJ, Ling Q, Zhou XH, Wang Y, Xie HY, Yu JR, et al. Urinary trypsin inhibitor attenuates hepatic ischemia-reperfusion injury by reducing nuclear factor-kappa B activation. Hepatobiliary Pancreat Dis Int 2009; 8: 53-58. PMID: 19208516.

22. Bao P, Gao W, Li S, Zhang L, Qu S, Wu C, et al. Effect of pretreatment with high-dose ulinastatin in preventing radiation-induced pulmonary injury in rats. Eur J Pharmacol 2009; 603: 114-119. PMID: 19101537.

23. Kim SJ, Yoo KY, Jeong CW, Kim WM, Lee HK, Bae HB, et al. Urinary trypsin inhibitors afford cardioprotective effects through activation of PI3K-Akt and ERK signal transduction and inhibition of p38 MAPK and JNK. Cardiology 2009; 114: 264-270. PMID: 19684396.

24. Matsuo O, Tanaka S, Kikuchi H. Effect of urinary trypsin inhibitor on osteoarthritis. Thromb Res 1988; 52: 237-245. PMID: 3143165.

25. Saitoh Y, Fujii Y, Oshima T. The ulinastatin-induced effect on neuromuscular block caused by vecuronium. Anesth Analg 1999; 89: 1565-1569. PMID: 10589650.

26. Mastumoto N, Ohara K, Yoshida N, Nakamura S, Nagasaki H, Aikawa K, et al. Protective effects of ulinastatin on hepatic oxygen metabolism during halothane anesthesia in the presence of graded hypoxic hypoxemia. Masui 1989; 38: 531-539. PMID: 2724518.

27. Aoike I, Takano Y, Gejyo F, Arakawa M. Ulinastatin gives rise to an effectual diursis in oliguric renal failure. Nephron 1989; 52: 368-369. PMID: 2770956.