Week 01 - Fatty Liver Disease - Moodle Version (1).pptx PDF

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This document is a presentation on fatty liver disease, outlining the definition

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Fatty Liver Disease
CMS200

Dr. Janis Li, ND
Learning Outcomes
1. Analyze the definition, epidemiology, classification, and diagnostic criteria of NAFLD and its
subtypes, including non-alcoholic steatohepatitis (NASH).
2. Interpret the risk factors and principal causes of NAFLD, such as obesity, diabetes,
hypertriglyceridemia, insulin resistance, and metabolic syndrome, considering that non-obese
individuals may also develop NAFLD.
3. Evaluate the role of maternal obesity, early-pregnancy glucose concentrations, gut dysbiosis, altered
bile acid metabolism, and genetic factors in NAFLD development, as well as the protective effect of
physical activity.
4. Correlate NAFLD with increased risk for cardiovascular disease, chronic kidney disease, colorectal
cancer, and liver complications, such as advanced hepatic fibrosis, cirrhosis, liver failure, and
hepatocellular carcinoma.
5. Compare the differences in NAFLD frequency and severity between genders and ethnicities, and
examine the association between NAFLD and insulin resistance.
6. Elucidate the clinical presentation, common symptoms, and laboratory abnormalities associated with
NAFLD, including elevated aminotransferase levels, hepatomegaly, and steatosis on
ultrasonography.
Learning Outcomes
7. Appraise the role of imaging studies, liver biopsy, and noninvasive tests for fibrosis in diagnosing
and evaluating NAFLD, as well as the importance of screening high-risk populations.
8. Determine when to refer a patient with NAFLD to a specialist and the importance of addressing and
treating comorbid conditions.
9. Evaluate the alternative designation "metabolic-associated (or metabolic dysfunction-associated)
fatty liver disease" (MAFLD) that has been proposed for NAFLD and the relationship between the
two conditions.
10.Assess the need for patient education regarding lifestyle changes, alcohol abstinence, and early
intervention to improve prognosis in patients with NAFLD.
11.Justify the importance of monitoring disease progression, screening for complications, and utilizing
an interprofessional approach to managing patients with NAFLD, including potential liver
transplantation in advanced cases.
12.Differentiate the grading and staging systems, differential diagnosis, and clinical scoring systems
used in NAFLD evaluation and management, as well as appraise the role of genetics and
environmental factors in NAFLD pathogenesis.
Non-Alcoholic Fatty Liver Disease
(NAFLD)
NAFLD is an umbrella term that includes a spectrum of
conditions characterized by:
Evidence of hepatic steatosis on imaging or histology
(macro-vesicular steatosis)
Exclusion of secondary causes of hepatic steatosis (e.g.,
significant alcohol consumption, chronic use of medications
that can cause hepatic steatosis, hereditary disorders)
Non-Alcoholic Fatty Liver Disease
(NAFLD)
A great introductory video available at
The Canadian Liver Foundation
NAFLD: Terminology Review
Steatosis: abnormal retention of fat (lipids) within an organ
Hepatic steatosis: fat accumulation in the liver
Hepatitis: inflammation of the liver
Steatohepatitis: fat accumulation and inflammation of the liver
Fibrosis: scarring
Cirrhosis: permanent liver damage (scar tissue replaces liver
cells)
Progression of NAFLD
Simple
steatosis or Non- NASH with
Non- alcoholic hepatocell
alcoholic steatohepa ular
fatty liver titis carcinoma
(NAFL) (NASH)

NAFL = 5% or
greater
hepatic
steatosis
without NASH = 5% or greater
hepatocellula hepatic steatosis plus
r injury or hepatocellular injury and
fibrosis inflammation, with or Signimu, CC BY-SA 3.0, via Wikimedia
without fibrosis
NAFLD: Epidemiology
Most common cause of liver disease in Canada
NAFLD prevalence: 20-30% in western countries
Affects ~20% of Canadians and ~37% of adult Americans
NASH prevalence 3-5%
More common in obese/overweight adults but can affect nonobese
individuals
Average age at diagnosis is 50 years
Rising childhood obesity  increasing prevalence in children
3-10% in children
NAFLD: Epidemiology
Hispanics > Caucasians > African Americans
In Caucasians, men > women (but no sex difference in
Hispanics and African-Americans)
NAFLD: Risk Factors and Causes
Principal causes:
Obesity (40% of patients with NAFLD)
Diabetes mellitus (>20% of patients with NAFLD)
Dyslipidemia/hypertriglyceridemia (>20% of patients
with NAFLD)

In association with insulin resistance and metabolic
syndrome
What is Metabolic Syndrome?
Meeting any 3 of the following criteria constitutes a diagnosis
of metabolic syndrome:
Blood pressure Systolic BP ≥ 130 mmHg or
Diastolic BP ≥ 85 mmHg or
Antihypertensive pharmacotherapy in a patient with a history
of hypertension
Fasting glucose ≥ 100 mg/dL (5.6 mmol/L) or
level Pharmacotherapy for elevated glucose level
High-density < 50 mg/dL (1.29 mmol/L) in women; < 40 mg/dL (1.04
lipoprotein (HDL) mmol/L) in men or
cholesterol level Pharmacotherapy for reduced high-density lipoprotein
cholesterol level
Triglyceride level ≥ 150 mg/dL (1.7 mmol/L) or
Pharmacotherapy for elevated triglyceride level
Waist ≥ 35 inches (89 cm) in women; ≥ 40 inches (102 cm) in men
NAFLD aka MAFLD
NAFLD is considered the liver manifestation of metabolic
syndrome
Strong association with metabolic syndrome has led to
new terminology:

Metabolic-associated (or
metabolic dysfunction-
associated) fatty liver disease
(MAFLD)
NAFLD: Risk Factors and Causes
Maternal risk factors:
Maternal obesity
High maternal early-pregnancy glucose concentrations

Maternal protective factors:
Breastfeeding >6 months (avoidance of early
supplemental milk formula)
Reduces NAFLD risk in offspring and in mother
NAFLD: Risk Factors and Causes
Exposures:
Drugs (corticosteroids, amiodarone, diltiazem,
methotrexate, tamoxifen, irinotecan, oxaliplatin,
antiretroviral therapy)
Toxins (vinyl chloride, carbon tetrachloride, yellow
phosphorus, inorganic arsenic exposure)
NAFLD: Risk Factors and Causes
Dietary and nutritional factors:
Excessive dietary fructose consumption
Malnutrition
Starvation and refeeding syndrome
Total parenteral nutrition
NAFLD: Risk Factors and Causes
Genetic factors (in up to 35% patients)
Polymorphisms of the gene encoding apolipoprotein C3
Polymorphisms of the patatin-like phospholipase domain-
containing 3 (PNPLA3) gene
Polymorphism of TM6SF2
Polymorphism of HSD17B13
Variants of MBOAT1 and GCKR
NAFLD: Risk Factors and Causes
Associated conditions:
Cushing syndrome
Hypopituitarism
Polycystic ovarian syndrome
Hypothyroidism
Hypobetalipoproteinemia (low apolipoprotein B and LDL cholesterol)
Obstructive sleep apnea
Gut dysbiosis
Altered bile acid metabolism
Cholecystectomy
Psoriasis
NAFLD: Protective Factors
Physical activity protects against the development of NAFLD
Why?
Brainstorming exercise
Given what you know about risk factors for the development
of NAFLD, what are some important questions you might
want to ask your patient as part of your history taking?
NAFLD: Timing and Clinical Course
Slowly progressive disease – silent liver disease when there is only
steatosis
Early stages (simple steatosis or NAFL) are reversible
NAFL  20% develop NASH  20% progress to cirrhosis  possible liver
failure and liver cancer
Risk factors for advanced hepatic fibrosis and cirrhosis:
Advanced age
Obesity
Diabetes mellitus
Strongest predictor of progression of NAFLD is the degree of inflammation
on the first liver biopsy
The natural history of nonalcoholic fatty liver disease depends on histopathology. Nonalcoholic fatty liver
(NAFL) progresses very slowly, if at all, when fat alone is present on liver biopsy. By contrast, the presence of
nonalcoholic steatohepatitis (NASH) is associated with a more accelerated progression to fibrosis.
(Reproduced with permission from Parekh S, Anania FA. Abnormal lipid and glucose metabolism in obesity:
implications for nonalcoholic fatty liver disease, Gastroenterology. 2007;132(6):2191–2207.)
Citation: Chapter 45 Nonalcoholic Fatty Liver Disease, Friedman S, Blumberg RS, Saltzman JR. Greenberger's CURRENT Diagnosis & Treatment Gastroenterology, Hepatology,
& Endoscopy, 4e; 2022. Available at: https://accessmedicine.mhmedical.com/content.aspx?bookid=3204&sectionid=266865566
Copyright © 2023 McGraw-Hill Education. All rights reserved
Progression of NAFLD

Signimu, CC BY-SA 3.0, via Wikimedia
NAFLD: Timing and Clinical Course
Complications:
Cardiovascular disease
Hepatocellular carcinoma (annual risk 1-2%)
End-stage liver disease and liver failure (develops over 10
years in 45% of patients)
NAFLD can coexist with other chronic liver conditions
Cardiovascular risk factors contribute to mortality in those with
end stage liver cirrhosis and hepatocellular carcinoma
NAFLD: Timing and Clinical Course
NAFLD also predicts risk of:
Cardiovascular events
Chronic kidney disease
Colorectal cancers
Type 2 diabetes mellitus

Mantovani, Alessandro et al. “Complications,
morbidity and mortality of nonalcoholic fatty liver
disease.” Metabolism: clinical and
experimental vol. 111S (2020): 154170.
NAFLD: Signs and Symptoms
Most are asymptomatic
Possible presentations in early stages:
Fatigue
Malaise
Mild abdominal discomfort: right upper quadrant
NAFLD: Signs and Symptoms What physical
exam
Possible presentations in advanced stages: technique(s)
can determine
Nausea Hepatomegaly (inthis?
75% of
Vomiting patients)
Jaundice Spider angiomas
Pruritis Signs of portal hypertension –
Memory impairment edema, ascites, caput medusae
Easy bleeding Palmar erythema
Loss of appetite Gynecomastia
Dupuytren contracture
Petechiae
Detecting Hepatomegaly
Diagnostic accuracy of physical exam findings:
Sensitiv Specific LR LR-
Physical Exam Finding
ity (%) ity (%) +
Midclavicular liver span ≥ 10 61-92 30-43 NS NS
cm on percussion
Palpable liver edge 39-71 56-85 1.9 0.6

McGee Steven R. Evidence-Based Physical Diagnosis. 4th edition 4th ed.
Diagnosing Hepatocellular Disease in
Patient with Jaundice
Diagnostic accuracy of physical exam findings:
Physical Exam Finding Sensitivity Specificity LR+ LR-
(%) (%)
Spider angiomas 35-47 88-97 4.7 0.6
Palmar erythema 49 95 9.8 0.5
Dilated abdominal veins 42 98 17.5 0.6
Ascites 44 90 4.4 0.6
Palpable spleen 29-47 83-90 2.9 0.7
Palpable gallbladder 0 69 0.04 1.4
Palpable liver 71-83 15-17 NS NS
Liver tenderness 37-38 70-78 NS NS
McGee Steven R. Evidence-Based Physical Diagnosis. 4th edition 4th ed.
Diagnosing Cirrhosis in Patients with
Chronic Liver Disease
Diagnostic accuracy of physical exam findings:
Physical Exam Finding Sensitivity Specificity LR+ LR-
(%) (%)
Spider angiomas 33-84 48-98 4.2 0.5
Palmar erythema 12-70 49-98 3.7 0.6
Gynecomastia 18-58 92-97 7.0 NS
Reduction of body or pubic hair 24-51 94-97 8.8 NS
Jaundice 16-44 83-99 3.8 0.8
Dilated abdominal wall veins 9-51 79-100 9.5 NS

McGee Steven R. Evidence-Based Physical Diagnosis. 4th edition 4th ed.
Diagnosing Cirrhosis in Patients with
Chronic Liver Disease
Diagnostic accuracy of physical exam findings:
Physical Exam Finding Sensitivity Specificity LR+ LR-
(%) (%)
Hepatomegaly 31-96 20-96 2.3 0.6
Palpable liver in epigastrium 50-86 68-88 2.7 0.3
Liver edge firm to palpation 71-78 71-90 3.3 0.4
Splenomegaly 5-85 35-100 2.5 0.8
Ascites 14-52 82-99 6.6 0.8
Peripheral edema 24-56 87-92 3.0 0.7
Encephalopathy (disordered 9-29 98-99 8.8 NS
consciousness and asterixis)

McGee Steven R. Evidence-Based Physical Diagnosis. 4th edition 4th ed.
Vascular spider telangiectasia. (Reproduced, with permission, from Sherlock S, Summerfield JA.
Color Atlas of Liver Disease. Mosby, 1991.)

Citation: 16-01 Jaundice & Evaluation of Abnormal Liver Biochemical Tests, Papadakis MA, McPhee SJ, Rabow MW, McQuaid KR. Current Medical Diagnosis & Treatment 2023;
2023. Available at: https://accessmedicine.mhmedical.com/content.aspx?bookid=3212&sectionid=269152700
Copyright © 2023 McGraw-Hill Education. All rights reserved
Palmar erythema in chronic liver disease. Palmar erythema refers to reddening of the palms,
specifically of the thenar and hypothenar eminences (arrows) and of the fingertips. This is a
consequence of elevated circulating estrogen levels in chronic liver disease. (Used, with
permission, from Neil Mehta, MD.)
Citation: 16-11 Cirrhosis, Papadakis MA, McPhee SJ, Rabow MW, McQuaid KR. Current Medical Diagnosis & Treatment 2023; 2023. Available at:
https://accessmedicine.mhmedical.com/content.aspx?bookid=3212&sectionid=269153543
Copyright © 2023 McGraw-Hill Education. All rights reserved
Caput medusae in cirrhosis. A consequence of portal hypertension, distended and engorged
superficial paraumbilical veins (arrows) that radiate from the umbilicus across the abdomen to
join systemic veins, are referred to as a caput medusa (Latin for "head of Medusa"). (Used, with
permission, from Neil Mehta, MD.)
Citation: 16-11 Cirrhosis, Papadakis MA, McPhee SJ, Rabow MW, McQuaid KR. Current Medical Diagnosis & Treatment 2023; 2023. Available at:
https://accessmedicine.mhmedical.com/content.aspx?bookid=3212&sectionid=269153543
Copyright © 2023 McGraw-Hill Education. All rights reserved
Ascites, gynecomastia. (Reproduced, with permission, from Sherlock S, Summerfield
JA. Color Atlas of Liver Disease. Mosby, 1991.)

Citation: 16-01 Jaundice & Evaluation of Abnormal Liver Biochemical Tests, Papadakis MA, McPhee SJ, Rabow MW, McQuaid KR. Current Medical Diagnosis & Treatment 2023;
2023. Available at: https://accessmedicine.mhmedical.com/content.aspx?bookid=3212&sectionid=269152700
Copyright © 2023 McGraw-Hill Education. All rights reserved
NAFLD: Differential Diagnosis
Viral hepatitis (hepatitis B, hepatitis C)
Alcoholic hepatitis
Autoimmune hepatitis
Hereditary hemochromatosis
Alpha-1 antitrypsin deficiency
Primary sclerosing cholangitis
Wilson disease
Primary biliary cholangitis
Cirrhosis
NAFLD: Further Testing
Labs to evaluate liver function: Liver enzymes
Alanine aminotransferase (ALT) and aspartate
aminotransferase (AST)
May be mildly elevated; normal in up to 80% patients
AST/ALT ratio < 0.8 (ALT/AST ratio > 1) in early NAFLD (in
contrast to alcohol associated liver disease where AST/ALT
ratio > 1.5); but AST may be > ALT (i.e., AST/ALT ratio
increases) as advanced fibrosis and cirrhosis develop
Alkaline phosphatase (ALP) and gamma-glutamyl transferase
(GGT) may also be elevated
NAFLD: Further Testing
Labs to examine for metabolic risk factors:
Lipid levels: cholesterol, triglycerides, high-density lipoprotein, low-density lipoprotein
Fasting glucose or HbA1C levels

Fasting glucose and fasting insulin levels can be used to calculate measures of insulin
resistance:
Homeostasis Model Assessment (HOMA)
Normal value < 3.99
Online calculator available at https://sasl.unibas.ch/11calculators-HOMA.php
Quantitative Insulin Sensitivity Check Index (QUICKI)
Normal value > 0.35
Online calculator available at https://sasl.unibas.ch/11calculators-QUICKI.php
NAFLD: Further Testing
Consider labs to exclude other causes of liver disease:
Condition Clinical Features Laboratory Evaluation
Alpha1- Hepatomegaly and elevated liver Alpha1-antitrypsin level,
antitrypsin enzyme levels phenotyping, liver biopsy
deficiency
Autoimmune More common in women and Antinuclear antibody, smooth muscle
hepatitis individuals with a history of thyroid antibody, liver/kidney microsomal
disease antibody testing
Hereditary Bronze diabetes (darkening of skin Complete blood count, ferritin level,
hemochromatosi and hyperglycemia), arthritis, transferrin saturations, genetic
s congestive heart failure, testing (HFE gene), liver biopsy with
impotence, family history staining for iron, MRI
Wilson disease Neurologic and psychological 24-hour urinary copper
presentation with liver disease at measurement, ceruloplasmin level,
young age (< 40 years), family liver biopsy, genetic testing
history
NAFLD: Further Testing
Imaging tests:
Ultrasonography: increased hepatic echogenicity
Imaging test of choice
Least invasive; relatively inexpensive; no exposure to
radiation
Computed tomography (CT) – unenhanced or contrast-
enhanced
Magnetic resonance imaging (MRI)
NAFLD: Further Testing
Diagnostic accuracy of imaging tests for the evaluation of
NAFLD:

Imaging Test Sensitivity Specificity PPV NPV LR+ LR-
(%) (%) (%) (%)
Ultrasonography 60-100 77-95 52-89 82-100 1.1-8.6 ∞-0.2
Unenhanced CT 88-95 90-99 79-98 95-98 2.7- 0.02-0.05
40.7
Contrast- 84-87 75-86 59-72 92-94 1.4-2.7 0.06-0.09
enhanced CT
MRI 96 93 85 98 5.9 0.02
Wilkins, Thad et al. “Nonalcoholic fatty liver disease:
diagnosis and management.” American family
physician vol. 88,1 (2013): 35-42.
https://www.aafp.org/pubs/afp/issues/2013/0701/p35.
html#afp20130701p35-t4
NAFLD: Further Testing
Comparing the diagnostic accuracy of imaging tests and liver
biopsy for the evaluation of NAFLD:
Test Sensitivity Specificity LR+ LR-
(%) (%)
Ultrasonography 82-100 95 18.2 0.09
CT Similar to ultrasonography
MRI 95 95 19 0.05
Liver biopsy (single biopsy for diagnosis 73 92 8.6 0.3
for NASH)
Liver biopsy (for advanced fibrosis) 7.7 0.16
Alexander J. Nonalcoholic fatty liver disease (NAFLD). In: Stern
SC, Cifu AS, Altkorn D. eds. Symptom to Diagnosis: An Evidence-
Based Guide, 4e. McGraw Hill; 2020. Accessed July 2023.
https://accessmedicine-mhmedical-com.ccnm.idm.oclc.org/conten
NAFLD: Further Testing
How do clinicians decide which patients require further testing
with imaging?
NAFLD: Further Testing
Clinical risk scoring systems
Noninvasive scoring systems to predict risk of NAFLD
Can be used to screen high-risk groups (such as those with
metabolic syndrome or T2DM) for NAFLD
Fatty liver index (FLI)
Lipid accumulation product (LAP) index
Hepatic steatosis index (HSI)
Nonalcoholic fatty liver disease in
metabolic syndrome patients
scoring system (NAFLD-MS)
NAFLD: Further Testing
Fatty Liver Index (FLI)
Noninvasive scoring system to diagnose fatty liver (e.g., NAFLD,
NASH, or alcoholic fatty liver)
Online calculator available via MDCalc
Calculation based on BMI, waist circumference, GGT and triglyceride
levels:

Fatty Liver Index (FLI) = ey / (1 + ey) × 100
Where y = 0.953 × ln (triglycerides, mg/dL) + 0.139 × BMI, kg/m2 + 0.718 ×
ln (GGT, U/L) + 0.053 × waist circumference, cm – 15.745
NAFLD: Further Testing
Fatty Liver Index (FLI)
Interpretation:

Fatty Liver Risk Diagnosis
Index
< 30 Low Fatty liver ruled
out
(LR = 0.2) Consider
30 to < 60 Indeterminate Fatty liver ultrasound
for
neither ruled in confirmation/
nor ruled out clarification
≥ 60 High Fatty liver ruled
NAFLD: Further Testing
NAFLD in Metabolic Syndrome Score (NAFLD-MS Score)
Clinical scoring system to predict development of NAFLD in
patients with metabolic syndrome
Clinical Predictors Point Scoring LR+ for
s NAFLD
BMI ≥ 25 kg/m2 1.5
< 3 points = 2.32
AST/ALT ratio ≥ 1 1
low risk of
ALT ≥ 40 U/L 2 NAFLD
Type 2 diabetes 1
mellitus
≥ 5 points = 7.77
Saokaew, Surasak et al. “Clinical risk scoring for predicting non-
high risk
alcoholic fatty of
liver disease in metabolic syndrome patients
Central obesity 1
(waist-to-hip ratio ≥ NAFLD
(NAFLD-MS score).” Liver international : official journal of the
International Association for the Study of the Liver vol. 37,10
0.9 in male and ≥ 0.8 (2017): 1535-1543.
NAFLD: Further Testing
Liver Biopsy:
Small sample of liver tissue removed with a biopsy needle and
examined under a microscope
Liver biopsy and histology is the gold standard for diagnosis
NASH diagnosis can only be established with liver biopsy
Biopsy Findings
Type
Type 1 Fatty liver alone; macrovesicular steatosis
Type 2 Fatty accumulation and lobar inflammation
Type 3 Fat accumulation and ballooning degeneration Diagnos
is of
Type 4 Fat accumulation, ballooning degeneration and either
Mallory hyaline or fibrosis NASH
Nonalcoholic steatohepatitis (NASH). Liver biopsy histology demonstrates
diffuse steatosis as well as ballooning degeneration of hepatocytes (circles).
(Used, with permission, from James P. Grenert, MD.)
Citation: 16-10 Nonalcoholic Fatty Liver Disease, Papadakis MA, McPhee SJ, Rabow MW, McQuaid KR. Current Medical Diagnosis & Treatment 2023; 2023. Available at:
https://accessmedicine.mhmedical.com/content.aspx?bookid=3212&sectionid=269153482
Copyright © 2023 McGraw-Hill Education. All rights reserved
 NAFLD: Further Testing
Grading and staging of NAFLD histological lesions:
Grade Findings Stag Findings
Grade 1 Steatosis up to 66%, occasional ballooning in es
(mild) zone 3, scattered polymorphs with or without Stage No fibrosis
lymphocytes, mild or no portal inflammation 0
Grade 2 Any degree of steatosis, obvious ballooning Stage Zone 3 perisinusoidal
(modera predominantly in zone 3, intralobular 1 fibrosis only
te) inflammation with polymorphs and chronic Stage Zone 3 perisinusoidal and
inflammation, and mild to moderate portal 2 periportal fibrosis
inflammation
Stage Bridging fibrosis
Grade 3 Panacinar steatosis, ballooning and obvious 3
(severe) disarray predominantly in zone 3, intralobular
inflammation with scattered polymorphs with Stage Cirrhosis
or without mild chronic and mild to moderate 4
portal inflammation
NAFLD: Further Testing
NAFLD Activity Score (NAS):
Used in NAFLD patients who have had a liver biopsy
Score based on histology results:
Steatosis grade
Lobular inflammation
Liver cell injury (ballooning)
Score correlates with steatohepatitis diagnosis but should not
be used to definitively diagnosis NASH
Online calculator available via MDCalc
NAFLD: Further Testing
But not all NAFLD patients need a liver biopsy!
Noninvasive tools can identify patients who have a higher
likelihood of developing fibrosis
Liver biopsy should be offered to patients who are at high risk
for having NASH and advanced fibrosis based on noninvasive
testing
Liver biopsy should be ordered if noninvasive tests produce an
indeterminate result
NAFLD patients with low risk of fibrosis based on noninvasive
testing do not require a liver biopsy
NAFLD: Further Testing
Noninvasive tests for liver fibrosis
Noninvasive tests/scoring systems to predict risk of fibrosis
May reduce the need for liver biopsy in patients with NAFLD
AST/ALT ratio (AAR) FibroTest (FibroSure)
AST/platelet count ratio index Fibrometer
(APRI)
BARD score Magnetic resonance elastography
Enhanced liver fibrosis (ELF) panel Nonalcoholic fatty liver disease
fibrosis score (NFS)
Fibrosis-4 (FIB-4) index Ultrasound elastography
(different techniques including
transient elastography and shear
 Diagnostic accuracy of noninvasive tests for liver fibrosis:
Test Cutoff Sensitivity Specificity PP NP LR LR-
(%) (%) V V +
(%) (%)
AST/ALT ratio 0.8 74 78 59 88 1.4 0.1
AST/platelet count ratio 1 27 89 51 49 1.1 0.4
BARD score 2 89 44 41 90 0.7 0.1
Enhanced liver fibrosis 10.5 100 98 96 100 21 0-∞
panel
FIB-4 1.3 85 65 51 91 1.0 0.1
FibroTest (FibroSure) 0.7 15 98 76 73 3.2 0.3
Fibrometer 0.8 79 96 89 91 8.5 0.0
9
Magnetic resonance 2.74 94 73 60 97 1.5 0.0
elastography kPa 4
NAFLD fibrosis score (NFS) -1.5 78 58 44 86 0.8 0.2
Wilkins, Thad et al. “Nonalcoholic fatty liver disease: diagnosis and management.” American family
physician vol. 88,1 (2013): 35-42.
NAFLD: Further Testing
NAFLD Fibrosis Score (NFS):
Used in NAFLD patients to estimate the amount of scarring in the liver
Score based on:
Age
BMI
Impaired fasting glucose or diabetes
AST
ALT
Platelet count
Albumin
Online calculator available via MDCalc
A high score (> 0.676) increases likelihood of advanced fibrosis (LR+ 16.5)
NAFLD: Further Testing
Fibrosis-4 (FIB-4) Index:
Used in patients with liver disease to estimate the amount of liver fibrosis and
need for a liver biopsy
Score based on:
Age
AST
ALT
Platelet count
Online calculator available via MDCalc
A high score (> 3.25) is likely to have advanced fibrosis (may need liver
biopsy); a low score (< 1.45) is unlikely to have advanced fibrosis
NAFLD: Further Testing
Ultrasound Elastography:
Measures liver stiffness and stage of liver fibrosis by measuring
the propagation velocity of ultrasound waves that pass through
the liver
Several types including transient elastography (FibroScan), point
shear wave elastography, and two-dimensional shear wave
elastography
Cut-off values for the different stages of liver fibrosis are
determined by the various ultrasound elastography techniques
and equipment manufacturers
Johari, Muhammad Izzad et al. “A Randomised Controlled Trial on the Effectiveness and Adherence of Modified Alternate-day
Calorie Restriction in Improving Activity of Non-Alcoholic Fatty Liver Disease.” Scientific reports vol. 9,1 11232. 2 Aug. 2019,
NAFLD: Management and Patient
Education
Interprofessional approach to encourage lifestyle changes and manage
comorbid conditions
Encourage:
Weight loss
Dietary fructose restriction
Increased dietary fiber
Moderate exercise (to reduce abdominal obesity)
Alcohol abstinence
Discontinuation of hepatotoxic drugs
Optimal treatment of diabetes and hyperlipidemia
NAFLD: Management and Patient
Education
NASH patients need to be followed by specialists (hepatologists
or gastroenterologists)
Liver transplantation may be required in NASH patients with
advanced cirrhosis
NAFLD is the second most common reason for liver
transplant in North America
NASH with cirrhosis requires surveillance for hepatocellular
carcinoma with a liver ultrasound every six months
Brainstorming exercise
When does a naturopathic doctor need to refer a patient with
NAFLD?
Suggested approach to NAFLD
Clinical Assess for likelihood of NAFLD
suspicion of
NAFLD
Obtain history, including an assessment for alcohol
Incidental intake, medication review, and family history of any
finding of liver conditions
hepatic Perform physical exam including calculating BMI and
steatosis on measuring waist circumference
imaging Order lab tests:
Liver function testing (i.e., liver enzyme levels such
Elevated liver as ALT, AST)
enzymes Fasting glucose or HbA1C
Lipid profile
Ferritin and iron/TIBC
Hepatitis B surface antigen (HBsAg) and hepatitis C
virus antibody (anti-HCV) testing
If LFTs are chronically elevated or family history is
positive for cirrhosis, consider other testing:
antinuclear antibody and smooth muscle antibody
Continued on next slide
testing; alpha1-antitrypsin and ceruloplasmin level;
 Continue to perform
Assess for likelihood of relevant investigations to
NAFLD unlikely
NAFLD determine alternative
cause for patient’s
signs/symptoms and/or
Obtain liver hepatic steatosis and/or
NAFLD highly
ultrasonography (if not elevated liver enzymes
likely
already performed)
If If AST/ALT ratio
AST/ALT