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Copyright ©The Author(s) 2015.
World J Gastroenterol. Oct 21, 2015; 21(39): 10982-10993
Published online Oct 21, 2015. doi: 10.3748/wjg.v21.i39.10982
Table 1 Methods used to define muscle mass or function in cirrhosis
MethodMeasurements obtainedLimitationsNotations
Multiple (four) compartment modelTotal body waterRequires combinations of methods (such as water dilution, densitometry)Best model for cirrhosis when fluid overload is present
Body fat
Fat free dry matter (protein)
Bone mineral content
Dual X-ray AbsorptiometryBody fat Fat free body mass Bone mineral contentLimited ability to differentiate between lean tissue and body water with excess body water resulting in overestimation of fat free mass[1]Peripheral measures of lean tissue are less impacted by ascites[24,26]
Ascites, especially more than 4 liters, can significantly impact truncal measures[26,27]
Cross sectional imagingEstimate skeletal muscle volumeCan be used to determine differences in skeletal muscle between groups[31] Studies use different muscle groups, anatomic levels and cutoff values to diagnose sarcopeniaMeasurements 5 cm above the level of the 4th-5th lumbar vertebra had the highest correlation with total body skeletal volume[31]
Biochemical methodsSkeletal muscle massTotal body protein is a measure of functional muscle mass and can be done through techniques such as in vivo neutron activation analysis 24 h urine creatinine is one method, but is limited in cirrhosis where renal insufficiency is common[93]Use calculations based on these methods to quantify muscle mass
Bioelectrical impedence analysisFat free mass Fat massGuidelines recommend against routine use of BIA under states of altered hydration[94]Segmental BIA was found to have a better correlation and lower standard error in estimating body cell mass in the setting of cirrhosis without ascites but still performs poorly with ascites present[95]
BIA estimates of total body water were found to be accurate in cirrhotic patients without ascites, but performed poorly when ascites was present[23]Phase angle can be used. In a study including participants with a wide range in severity of liver disease, phase angle was positively correlated with total body protein, muscle mass and muscle strength[96]
AnthropometryEstimate muscle massEdema alters results of anthropometry overestimating muscle mass[8]Mid arm circumference was found to be one of the most accurate anthropometric measures[29] and was most predictive of clinical outcomes[97]
Functional MeasuresMeasures ability to perform physical task, for which muscle function is one componentCommon functional measures assess all systems involved in exercise including cardiovascular, pulmonary, hematologic, neurologic and musculoskeletal[33]Include tests such as submaximal cardiopulmonary fitness tests, six minute walk test, hand grip strength and isokinetic strength of flexion and extension at different joints Often simple tests such as hand grip correlate with measures of skeletal muscle[29]
BIA: Bioelectrical impedance analysis.
Table 2 Measures, definitions and outcomes relating to sarcopenia in the setting of cirrhosis and liver transplant
StudyMethodDefinitions used/proposedOutcomesNotes/Limitations
Selberg et al[96]BIA, phase angle> 5.4° normal 4.4°-5.4 borderline < 4.4° abnormalPhase angle < 5.4° associated with significantly lower survivalPhase angle may remain normal in cases of severe tissue loss when proportional losses of extracellular mass and body cell mass may occur
Kaido et al[11]BIA, multiphase device (InBody 720; BioSpace, Tokyo, Japan)< 90% skeletal muscle mass compared to standard or body cell mass below 23.0 kgSurvival was significantly decreased in recipients with low skeletal muscle mass or low body cell massNo data is provided on volume status, although Child-Pugh classification is given
Percent skeletal muscle mass against a standard and calculated body cell massNutritional supplementation with branched chain amino acids improved survival in those with low skeletal muscle mass
Englesbe et al[15]CT, combined area of right and left psoas muscle area at the highest level of the 4th lumbar vertebra Control population was 248 trauma patientsPercentile cutoffs for total psoas area in transplant population 1910 mm2 50th percentile 1420 mm2 25th percentile 950 mm2 5th percentileDecreased psoas muscle area associated with higher risk of mortality 25th percentile HR = 1.88 5th percentile HR = 3.46Retrospective definitions of sarcopenia were not derived from the control trauma patients, but were based on percentiles from the transplant population Included CT scans either 90 d before or after transplant; majority of scans were after transplant
Tandon et al[12]CT or MRI, cross sectional area of muscle at 3rd lumbar vertebra (psoas, paraspinals, transversus abdominis, rectus abdominis and internal and external obliques)Total L3 skeletal muscle area ≤ 52.4 cm2/m2 in males ≤ 38.5 cm2/m2 in femalesSarcopenia present in 41% of wait listed candidates Higher wait-list mortality with sarcopenia (HR = 2.36, 95%CI: 1.23-4.53) Greatest effect was in those with low MELD scoreRetrospective Only study to report use of both MRI and CT
Montano-Loza et al[18]CT cross sectional area of muscle at 3rd lumbar vertebra (psoas, paraspinals, transversus abdominis, rectus abdominis and internal and external obliques) Muscle identified by Housfield unit between -29 and + 150Total L3 skeletal muscle area ≤ 52.4 cm2/m2 in males ≤ 38.5 cm2/m2 in femalesSarcopenia present in 40% of cirrhotics Sarcopenia was independent risk factor for mortality (HR = 2.28, P = 0.008) One year survival for cirrhosis with sarcopenia was 53% compared to 83% in cirrhosis without sarcopeniaProspective data
Hamaguchi et al[14]CT, cross sectional psoas muscle area at level of umbilicus Intramuscular fat accumulation of multifidus muscle (multifidus muscle Housfield units/subcutaneous fat Housfield units)ROC curves selected from study data for best accuracy in predicting death Intramuscular adipose tissue content -0.375 in males and -0.216 in females Psoas muscle mass normalized for height ≤ 6.868 cm2/m2 in males ≤ 4.117 cm2/m2 in femalesPretransplant increased intramuscular adipose tissue content (OR = 3.898, 95%CI: 2.025-7.757) and decreased psoas muscle mass (OR = 3.635, 95%CI: 1.896-7.174) were associated with mortalityUsed umbilical level which can vary based on body habitus Constructed cutoffs based on diseased population Included intramuscular fat content as a measure of muscle quality
Tsien et al[13]CT cross sectional at mid 4th vertebra levelPsoas muscle area normalized 5th percentile cutoffs ≤ 12.27 cm2/m2 in males less than 50 yr of ageSarcopenia was seen in 62.3% prior to transplant and increased to 86.8% after transplantIncludes serial measures in the same patients
Total cross sectional area of psoas, paraspinals and abdominal wall muscles (rectus abdominis, oblique and transversus abdominis) normalized to height ≤ 10.12 cm2/m2 in males more than 50 yr of age ≤ 10.47 cm2/m2 in females less than 50 yr of age ≤ 10.33 cm2/m2 in females more than 50 yr of ageOnly 6.1% had reversal of sarcopenia after transplant and 75% without pretransplant sarcopenia developed it after transplantMean time from transplant to post-transplant CT was about one year (13.1 ± 8.0 mo)
Reference ranges derived from 109 healthy control subjects undergoing CT for unspecified abdominal painTotal abdominal muscle area normalized 5th percentile cutoffs ≤ 60.09 cm2/m2 in males less than 50 yr of age ≤ 48.97 cm2/m2 in males more than 50 yr of age ≤ 53.43 cm2/m2 in females less than 50 yr of age ≤ 41.28 cm2/m2 in females more than 50 yr of ageReduction in muscle after transplant was associated with new onset diabetes mellitusSince follow up scan was done for indications (ie HCC surveillance, infection, pain, increased aminotransferases) the potential for significant selection bias exists
Masuda et al[9]Cross sectional CT of psoas muscle at L3 Calculated area by multiplying major and minor axis of psoas (a × b ×∏)< 800 cm in men < 380 cm in women3 and 5 yr survival with sarcopenia was 74.5% and 69.7% respectively, without sarcopenia was 88.9% and 85.4% respectively (P = 0.02)Enteral nutrition given in immediate post operative period appeared to decrease risk of sepsis when sarcopenia was present
Compared to a reference group of healthy donorsSepsis was seen in 17.7% with sarcopena, 7.4% without sarcopenia (P = 0.03)
MELD: Model for end stage liver disease; CT: Computed tomography.
Table 3 Methods and outcomes when measuring muscle function in the setting of cirrhosis and liver transplant
StudyMethodOutcomesNotes/limitations
Andersen et al[37]Isokinetic strength of flexion and extension of six jointsUpper and lower extremity strength was decreased in cirrhotics vs controlsOnly included patients with alcohol related cirrhosis
Lower extremity strength was associated with lean body mass and mid arm circumference, an effect independent of severity of liver disease, neuropathy, biochemical data and recent alcohol useThe majority of patients had Child-Pugh A or B classification Included 24 cirrhotics and 24 controls
Tarter et al[98]Isokinetic strength measured by upper and lower extremity peak force, peak torque, total work and powerMost measures of strength were decreased in cirrhotic patients vs controlsStudy included 49 with alcoholic cirrhosis, 42 with non-acoholic cirrhosis and 50 controls
There was no difference in any measure between those with alcohol vs non-alcohol related cirrhosisNo patient had consumed alcohol in greater than one year prior to testing
Beyer et al[35]Maximal oxygen uptake measured on a cycle ergometer SMWT Isokinetic knee flexion and extensionMaximal oxgen uptake, SMWT and isokinetic knee strength increased over the first six months after transplant compared to pretransplant values No changes were noted between six and 12 mo after transplantSmall study with only 17 patients having post transplant data and 13 patients completing both pretransplant and posttransplant assessment of maximal oxygen uptake Used a supervised exercise program after transplant
Epstein et al[38]Symptom limited cardiopulmonary testing on a cycle ergometerWhen examining patients that went on to transplant, a significantly higher proportion of patients that died within the first 100 post-operative days had a peak oxygen consumption < 60% predicted and had oxygen consumption at the anaerobic threshold < 50% predicted peak oxygen consumptionMedian MELD at the time of exercise testing was low (7-12) The median time from exercise testing to transplant was long (471 ± 300 d)
Prentis et al[39]Symptom or exertional limited cardiopulmonary testing on a cycle ergometerSixty tested patients went on to liver transplant with a 10% 90 d mortalityMean MELD at transplant was low (< 20)
Mean aerobic threshold was higher in survivors and was only variable in multivariate analysis that was associated with mortalityCompared to above study (Epstein 2004[38]), the authors did not make comparisons to population based reference values, but used ROC curve analysis to define thresholds associated with outcomes
Optimal anaerobic threshold associated with survival was > 9 mL/min per kg
Anaerboic threshold > 11 mL/min per kg was associated with shorter stay in critical care setting
Carey et al[34]Six minute walk testCandidates awaiting liver transplant had decreased SMWT distance (369 ± 122 m), significantly lower than reference valuesIncluded patients too ill to walk, and designated zero m for this group
When controlling for other factors including age and MELD, SMWT distance was significantly associated with wait list mortality (HR = 0.58, 95%CI: 0.37-0.93)
ROC analysis found cut off value of 250 m having the highest sensitivity and specificity for mortalityDesignated patients removed from the list as a waitlist death
Alameri et al[36]Six minute walk testPatients with cirrhosis had significantly diminished SMWT distance (306 ± 111 vs 421 ± 47 m, P < 0.0001)Used Child-Pugh to assess severity of liver disease, no data on MELD
SMWT was an independent predictor of survival and was inversely correlated with Child-Pugh classification
The lowest quartile walked < 250 m
SMWT: Six minute walk test; MELD: Model for end stage liver disease.