Easl clinical practice guidelines on the management of ascites, spontaneous bacterial peritonitis, and hepatorenal
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quinolone to prevent the development of SBP (Level A1). 3.3.2. Patients with low total protein content in ascitic fluid without prior history of spontaneous bacterial peritonitis Cirrhotic patients with low ascitic fluid protein concentration (<10 g/L) and/or high serum bilirubin levels are at high risk of Clinical Practice Guidelines 406 Journal of Hepatology 2010 vol. 53 j 397–417
developing a first episode of SBP [10,149–152]. Several studies have evaluated prophylaxis with norfloxacin in patients without prior history of SBP (Table 7) [153–157]. One pilot, randomized, open-label trial was performed comparing primary continuous prophylaxis with norfloxacin to inpatient-only prophylaxis in 109 patients with cirrhosis and ascitic fluid total protein level 6 15 g/L or serum bilirubin level >2.5 mg/dl [154]. SBP was reduced in the continuous treatment group at the expense of more resistance of gut flora to norfloxacin in that group. In another study, 107 patients with ascitic fluid total protein level
norfloxacin (400 mg/day for 6 months) or placebo [155]. Of note, the existence of severe liver failure was not an inclusion crite- rion. The primary endpoint was the occurrence of GNB infec- tions. Norfloxacin significantly decreased the probability of developing GNB infections, but had no significant effect on the probability of developing SBP or survival. However, in this trial, the sample size was not calculated to detect differences in survival. In a third investigation, 68 patients with cirrhosis and low ascites protein levels (<15 g/L) with advanced liver fail- ure [Child-Pugh score P9 points with serum bilirubin level P 3 mg/dl or impaired renal function (serum creatinine level P 1.2 mg/dl, blood urea nitrogen level P25 mg/dl, or serum sodium level 6130 mEq/L)] were randomized in a double-blind, placebo-controlled trial, to receive norfloxacin (400 mg/day for 12 months) or placebo [156]. The primary endpoints of the trial were 3-month and 1-year survival. Norfloxacin significantly improved the 3-month probability of survival (94% versus 62%; p = 0.03) but at 1 year the difference in survival was not significant (60% versus 48%; p = 0.05). Norfloxacin administra- tion significantly reduced the 1-year probability of developing SBP (7% versus 61%) and HRS (28% versus 41%). In a fourth study, 100 patients with ascitic fluid total protein level <15 g/ L were randomized in double-blind, placebo-controlled trial to ciprofloxacin (500 mg/day for 12 months) or placebo [157]. Enrolled patients had moderate liver failure (the Child-Pugh scores were 8.3 ± 1.3 and 8.5 ± 1.5, in the placebo and ciproflox- acin group, respectively). The primary endpoint was the occur- rence of SBP. Although SBP occurred in 2 (4%) patients of the ciprofloxacin group and in 7 (14%) patients of the placebo group, this difference was not significant. Moreover, the probability of being free of SBP was not significant (p = 0.076). The probability of remaining free of bacterial infections was higher in patients receiving ciprofloxacin (80% versus 55%; p = 0.05). The probabil- ity of survival at 1 year was higher in patients receiving cipro- floxacin (86% versus 66%; p < 0.04). Nevertheless, a type II error cannot be ruled out as the sample size was not calculated to detect differences in survival. The duration of primary antibi- otic prophylaxis has not been established. Recommendations One double-blind, placebo-controlled, randomized trial performed in patients with severe liver dis- ease (see text) with ascitic fluid protein lower than 15 g/L and without prior SBP showed that norfloxacin (400 mg/day) reduced the risk of SBP and improved survival. Therefore, these patients should be considered for long-term prophylaxis with norfloxacin (Level A1). In patients with moderate liver disease, ascites protein concentration lower than 15 g/L, and without prior history of SBP, the efficacy of quinolones in preventing SBP or improv- ing survival is not clearly established. Studies are needed in this field. 3.3.3. Patients with prior spontaneous bacterial peritonitis In patients who survive an episode of SBP, the cumulative recurrence rate at 1 year is approximately 70% [108]. The prob- ability of survival at 1 year after an episode of SBP is 30–50% and falls to 25–30% at 2 years. Therefore, patients recovering from an episode of SBP should be considered for liver trans- plantation. There is only one randomized, double-blind, pla- cebo-controlled trial of norfloxacin (400 mg/day orally) in patients who had a previous episode of SBP [158] (Table 7). Table 7. Antibiotic therapy for prophylaxis of spontaneous bacterial peritonitis (SBP) in patients with cirrhosis. a Reference Type of prophylaxis Treatments Number of patients
Number of GNB b infections p-value Incidence of SBP n (%) p-value
Ginès, 1990 [158]
Enrolled only patients with prior SBP c Norfloxacin versus placebo 40 1 – 5 (12)
0.02 40 10 14 (35) Soriano, 1991 [153] Enrolled patients without prior SBP and patients with prior SBP d Norfloxacin versus no treatment 32 0 <0.001 0 (0)
<0.02 31 9 7 (22.5) Singh, 1995 [161] Enrolled patients without prior SBP and patients with prior SBP d Trimethoprim–sulfamethoxazole versus no treatment 30 9 – 1 (3)
0.03 30 0 8 (27) e Rolachon, 1995 [160] Enrolled patients without prior SBP and patients with prior SBP c Ciprofloxacin versus placebo 28 1 – 1 (4)
<0.05 32 0 7 (22) Novella, 1997 [154] Enrolled only patients without prior SBP d Continuous norfloxacin versus in patient-only prophylaxis 56 11
1 (1.8) <0.01 53 13 9 (16.9) Grangé, 1998 [155] Enrolled only patients without prior SBP c Norfloxacin versus placebo 53 0 <0.04 0 (0)
NA 54 6 5 (9) Fernández, 2007 [156] Enrolled only patients without prior SBP c Norfloxacin versus placebo 35 13 – 2 (6)
0.02 33 6 10 (30) Terg, 2008 [157] Enrolled only patients without prior SBP c Ciprofloxacin versus placebo 50 – – 2 (4)
0.076 50 7 (14) NA, not available. a Studies appear in chronological order. b GNB means Gram-negative bacteria. c Randomized, double-blind, placebo-controlled trial. d Randomized, unblinded trial. e Including one patient with spontaneous bacteremia due to Klebsiella pneumonia. JOURNAL OF HEPATOLOGY Journal of Hepatology 2010 vol. 53 j 397–417
407 Treatment with norfloxacin reduced the probability of recur- rence of SBP from 68% to 20% and the probability of SBP due to GNB from 60% to 3%. Survival was not an endpoint of this study. In an open-label, randomized study comparing norfloxa- cin 400 mg/day to rufloxacin 400 mg/week in the prevention of SBP recurrence, 1-year probability of SBP recurrence was 26% and 36%, respectively (p = 0.16) [159]. Norfloxacin was more effective in the prevention of SBP recurrence due to Enterobac- teriaceae (0% versus 22%, p = 0.01). Three other studies assessed the effects of ciprofloxacin, trimethoprim–sulfameth- oxazole, and norfloxacin, but they included patients with and without previous episodes of SBP [153,160,161] (Table 7). All studies showed a reduced incidence of SBP with antibiotic prophylaxis. It is uncertain whether prophylaxis should be continued with- out interruption until liver transplantation or death in all patients with prior SBP or if treatment could be discontinued in patients showing an improvement of liver disease. Recommendations Patients who recover from an episode of SBP have a high risk of developing recurrent SBP. In these patients, the administration of prophylactic antibiotics reduces the risk of recurrent SBP. Norfloxacin (400 mg/day, orally) is the treatment of choice (Level A1). Alternative anti- biotics include ciprofloxacin (750 mg once weekly, orally) or co-trimoxazole (800 mg sulfamethoxazole and 160 mg tri- methoprim daily, orally), but evidence is not as strong as that with norfloxacin (Level A2). Patients who recover from SBP have a poor long-term sur- vival and should be considered for liver transplantation (Level A1).
3.3.4. Issues with prolonged antibiotic prophylaxis As mentioned earlier, prolonged antibiotic prophylaxis (primary or secondary) has led to the emergence of GNB resistant to quin- olones and even to trimethoprim/sulfamethoxazole [106]. In addition, there is an increased likelihood of infections from Gram-positive bacteria in patients who have received long-term SBP prophylaxis [156,162]. This underlines the need to restrict the use of prophylactic antibiotics to patients with the greatest risk of SBP. Common sense would suggest that quinolone prophy- laxis should be discontinued in patients who develop infection due to quinolone-resistant bacteria. However, there are no data to support this. 4. Hyponatremia Hyponatremia is common in patients with decompensated cir- rhosis and is related to impaired solute-free water excretion sec- ondary to non-osmotic hypersecretion of vasopressin (the antidiuretic hormone), which results in a disproportionate reten- tion of water relative to sodium retention [163–166]. Hyponatre- mia in cirrhosis is arbitrarily defined when serum sodium concentration decreases below 130 mmol/L [163], but reductions below 135 mmol/L should also be considered as hyponatremia, according to recent guidelines on hyponatremia in the general patient population [167]. Patients with cirrhosis may develop two types of hyponatre- mia: hypovolemic and hypervolemic. Hypervolemic hyponatre- mia is the most common and is characterized by low serum sodium levels with expansion of the extracellular fluid volume, with ascites and edema. It may occur spontaneously or as a con- sequence of excessive hypotonic fluids (i.e., 5% dextrose) or sec- ondary to complications of cirrhosis, particularly bacterial infections. By contrast, hypovolemic hyponatremia is less com- mon and is characterized by low serum sodium levels and absence of ascites and edema, and is most frequently secondary to excessive diuretic therapy. Serum sodium concentration is an important marker of prog- nosis in cirrhosis and the presence of hyponatremia is associated with an impaired survival [64,65,168–174]. Moreover, hypona- tremia may also be associated with an increased morbidity, par- ticularly neurological complications, and reduced survival after transplantation [175–177], although results of studies show dis- crepant findings with respect to survival. 4.1. Management of hyponatremia It is generally considered that hyponatremia should be treated when serum sodium is lower than 130 mmol/L, although there is no good evidence as to what is the level of serum sodium in which treatment should be started. The treatment of hypovolemic hyponatremia consists of administration of sodium together with identification of the causative factor (usually excessive diuretic administration) and will not be considered further in these guidelines. The key of the management of hypervolemic hyponatremia is to induce a negative water balance with the aim of normalizing the increased total body water, which would result in an improvement of serum sodium concentration. Fluid restriction has been the standard of care but is seldom effective. It is the clinical experience that fluid restriction is helpful in preventing a further decrease in serum sodium levels, although it is rarely effective in improving serum sodium concentration. The lack of efficacy is probably due to the fact that in practice total daily fluid intake cannot be restricted to less than 1 L/day. Although hypertonic sodium chloride administration has been used commonly in severe hypervolemic hyponatremia, its effi- cacy is partial, usually short-lived, and increases the amount of ascites and edema. The administration of albumin appears to improve serum sodium concentration, but more information is needed [178,179]. The pathophysiologically-oriented treatment of hyponatremia consists of improving solute-free water excretion which is mark- edly impaired in these patients. Early attempts using agents such as demeclocycline or j -opioid agonists were unsuccessful because of side effects [180–183]. In recent years, the pharmaco- logical approach to treatment of hypervolemic hyponatremia has made a step forward with the discovery of vaptans, drugs that are active orally and cause a selective blockade of the V2-receptors of AVP in the principal cells of the collecting ducts [184–186]. These drugs are effective in improving serum sodium concentration in conditions associated with high vasopressin levels, such as the syndrome of inappropriate antidiuretic hormone secretion (SIADH), heart failure, or cirrhosis [101,184,187–191]. The results of these studies consistently demonstrate that the administration of vaptans for a short period of time (1 week to 1 month in most of the studies) is associated with an increased urine volume and solute-free water excretion and improvement of the low serum sodium levels in 45–82% of patients. No significant changes have been observed in renal function, urine sodium, circulatory func- tion, and activity of the renin–angiotensin–aldosterone system. Clinical Practice Guidelines 408
Journal of Hepatology 2010 vol. 53 j 397–417 The most frequent side effect is thirst. Potential theoretical con- cerns of the administration of vaptans in patients with cirrhosis include hypernatremia, dehydration, renal impairment, and osmotic demyelination syndrome owing to a too rapid increase in serum sodium concentration. However, in the studies reported, the frequency of hypernatremia, dehydration, and renal impair- ment has been very low and no case of osmotic demyelination syndrome has been reported. Nevertheless, these complications should be taken into account and treatment should always be started in the hospital with close clinical monitoring and assess- ment of serum sodium levels, to avoid increases of serum sodium of more than 8–10 mmol/L/day. Vaptans should not be given to patients in an altered mental state (i.e., encephalopathy) who cannot drink appropriate amounts of fluid because of the risk of dehydration and hypernatremia. Vaptans are metabolized by CYP3A enzymes in the liver; therefore, drugs that are strong inhibitors of CYP3A such as ketoconazole, grapefruit juice, and clarithromycin among others, increase the exposure to vaptans and may be associated with large increases in serum sodium con- centration. Conversely, drugs that are inducers of the CYP3A sys- tem, such as rifampin, barbiturates, and phenytoin, may decrease the effectiveness of vaptans. Tolvaptan has been recently approved in the USA for the man- agement of severe hypervolemic hyponatremia (<125 mmol/L) associated with cirrhosis, ascites, heart failure, and the SIADH. In Europe the drug is currently only licensed for the treatment of SIADH. Conivaptan is also approved in the USA for the short- term (5 day) intravenous treatment of hypervolemic hyponatre- mia associated with different conditions. Treatment of tolvaptan is started with 15 mg/day and titrated progressively to 30 and 60 mg/day, if needed, according to changes in serum sodium con- centration. In randomized studies, a slightly increased frequency of gastrointestinal bleeding was reported in patients receiving tolvaptan compared to that in patients treated with placebo. No differences in the incidence of other side effects were observed. Nevertheless, it should be pointed out that tolvaptan was given for a period of 1 month and only limited long-term safety data exists with the use of this drug. Long-term, placebo-controlled studies in patients with cirrhosis treated with tolvaptan are clearly needed. No prospective evaluation on the efficacy and safety of conivaptan has been performed in patients with cirrho- sis and hyponatremia. As discussed previously, a phase-3 randomized double-blind placebo-controlled study comparing the efficacy of long-term treatment with satavaptan in combination with diuretics aimed at preventing ascites recurrence in patients with cirrhosis follow- ing LVP showed an increased frequency of complications and reduced survival in patients receiving satavaptan compared to those receiving placebo [104]. Recommendations It is important to differentiate hypovole- mic from hypervolemic hyponatremia. Hypovolemic hypona- tremia is characterized by low serum sodium concentrations in the absence of ascites and edema, and usually occurs after a prolonged negative sodium balance with marked loss of extracellular fluid. Management consists of administration of normal saline and treatment of the cause (usually diuretic withdrawal) (Level A1). Fluid restriction to 1000 ml/day is effective in increasing serum sodium concentration in only a minority of patients with hypervolemic hyponatremia, but may be effective in pre- venting a further reduction in serum sodium levels (Level A1). There are no data to support the use of either normal or hypertonic saline in the management of hypervolemic hypo- natremia (Level A1). Albumin administration might be effec- tive but data are very limited to support its use currently (Level B2). Treatment with vaptans may be considered in patients with severe hypervolemic hyponatremia (<125 mmol/L). Tolvaptan is licensed in some countries for oral treatment. Conivaptan is only licensed in some countries for short-term intravenous treatment. Treatment with tolvaptan should be started in the hospital and the dose titrated to achieve a slow increase in serum sodium. Serum sodium should be monitored closely particularly during the first days of treatment and whenever the dose of the drug is increased. Rapid increases in serum sodium concentration (>8–10 mmol/day) should be avoided to prevent the occurrence of osmotic demyelination syn- drome. Neither fluid restriction nor administration of saline should be used in combination with vaptans to avoid a too rapid increase in serum sodium concentration. Patients may be discharged after serum sodium levels are stable and no fur- ther increase in the dose of the drug is required. Concomitant treatment with drugs that are either potent inhibitors or inducers of the CYP3A should be avoided. The duration of treatment with vaptans is not known. Safety has only been established for short-term treatment (1 month) (Level B1). 5. Hepatorenal syndrome 5.1. Definition and diagnosis of hepatorenal syndrome Hepatorenal syndrome (HRS) is defined as the occurrence of renal failure in a patient with advanced liver disease in the absence of an identifiable cause of renal failure [56]. Thus, the diagnosis is essentially one of exclusion of other causes of renal failure. In 1994 the International Ascites Club defined the major criteria for the diagnosis of HRS and designated HRS into type 1 and type 2 HRS [56]. These were modified in 2007 [192]. The new diagnos- tic criteria are shown in Table 8. Various new concepts have emerged since the first definition and criteria for HRS were pub- lished in 1996 [56]. These are that vasodilatation mainly occurs in the splanchnic arterial bed, that the cardiac output in patients with HRS may be low or normal (infrequently high), but insuffi- cient for the patient’s needs, that the most important trigger for the development of type 1 HRS is bacterial infection, and that renal function can be improved by drug therapy [192]. Table 8. Criteria for diagnosis of hepatorenal syndrome in cirrhosis. Cirrhosis with ascites Serum creatinine >1.5 mg/dl (133 l mol/L)
Absence of shock Absence of hypovolemia as defined by no sustained improvement of renal function (creatinine decreasing to <133 l mol/L) following at least 2 days of diuretic withdrawal (if on diuretics), and volume expansion with albumin at 1 g/kg/day up to a maximum of 100 g/day No current or recent treatment with nephrotoxic drugs Absence of parenchymal renal disease as defined by proteinuria <0.5 g/day, no microhaematuria (<50 red cells/high powered field), and normal renal ultrasonography JOURNAL OF HEPATOLOGY Journal of Hepatology 2010 vol. 53 j 397–417
409 There are 2 types of HRS. Type 1 HRS is a rapidly progressive acute renal failure that frequently develops in temporal relation- ship with a precipitating factor for a deterioration of liver function Yüklə 2,55 Mb. Dostları ilə paylaş:
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