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Nonalcoholic Fatty Liver Disease (MASLD): What Blood Tests Can Reveal

Learn how liver enzymes, metabolic biomarkers, and fibrosis-risk calculations may help identify silent fatty liver risks and guide appropriate follow-up.
July 13, 2026
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Contents

Nonalcoholic fatty liver disease is a condition in which excess fat accumulates in the liver when the buildup is not primarily explained by heavy alcohol consumption. The condition is now more commonly called metabolic dysfunction-associated steatotic liver disease, or MASLD, because it is closely associated with insulin resistance, excess abdominal fat, abnormal cholesterol or triglycerides, high blood pressure, prediabetes, and type 2 diabetes.

MASLD is often silent. A person may feel well while liver fat, inflammation, or fibrosis—scar tissue—develops gradually. Blood testing cannot independently confirm how much fat or scarring is present in the liver. However, it can reveal liver-cell injury, metabolic risk factors, possible alternative causes of abnormal liver results, and information used in fibrosis-risk calculations.

Ulta Lab Tests provides direct access to many relevant blood tests, including a Nonalcoholic Fatty Liver Disease Base Assessment and a Nonalcoholic Fatty Liver Disease Advanced Assessment. These testing options can help patients gather objective information for more informed conversations with qualified healthcare providers.

Medical disclaimer: Lab testing provides health information but does not replace professional medical evaluation, diagnosis, imaging, or treatment. Results should be reviewed with a qualified healthcare provider.

Square infographic comparing a healthy liver with a fatty liver affected by nonalcoholic fatty liver disease, now called MASLD, alongside ALT, AST, A1c, glucose, lipid panel, and fibrosis-risk blood test graphics.
onalcoholic fatty liver disease, now commonly called MASLD, may be associated with abnormal liver enzymes, insulin resistance, elevated glucose, high triglycerides, and increased fibrosis risk. Blood tests can provide useful information for discussion with a healthcare provider.

Key Takeaways

  • Nonalcoholic fatty liver disease is now commonly called MASLD, while the inflammatory form previously called NASH is now called MASH.
  • MASLD is strongly associated with insulin resistance, obesity, prediabetes, type 2 diabetes, high triglycerides, low HDL cholesterol, and high blood pressure.
  • Most people have few or no early symptoms, and normal ALT or AST levels do not completely exclude fatty liver or significant fibrosis.
  • Blood tests can evaluate liver enzymes, glucose regulation, cholesterol, triglycerides, iron status, platelets, and other factors related to liver health.
  • FIB-4 uses age, AST, ALT, and the platelet count from a CBC with Differential and Platelets to estimate the probability of advanced fibrosis. It is a risk-stratification tool, not a diagnosis.
  • Ultrasound, transient elastography, magnetic resonance imaging, or occasionally liver biopsy may be needed when blood results or risk factors warrant further evaluation.
  • No single laboratory result should usually be interpreted in isolation.

What Is Nonalcoholic Fatty Liver Disease?

Nonalcoholic fatty liver disease describes excess fat stored inside liver cells. Under the newer terminology, MASLD is generally identified when liver steatosis is present along with at least one cardiometabolic risk factor and other important causes of liver fat have been considered.

The liver normally processes nutrients, produces proteins, regulates cholesterol, stores energy, and helps remove substances from the bloodstream. When more fatty acids reach or are produced by the liver than it can process or export, fat may begin accumulating within liver cells.

Understanding the New Fatty Liver Terminology

Previous TermCurrent TermGeneral Meaning
NAFLDMASLDLiver fat associated with metabolic dysfunction
Simple fatty liver or NAFLMASLSteatosis with little or no evident inflammation
NASHMASHSteatosis accompanied by liver-cell injury and inflammation
NAFLD with fibrosisMASLD with fibrosisFatty liver accompanied by increasing scar tissue
NASH cirrhosisMASH-related cirrhosisAdvanced and extensive liver scarring

The change from NAFLD to MASLD places greater emphasis on the metabolic factors that commonly contribute to the condition. It also recognizes that metabolic dysfunction and alcohol exposure can overlap. A careful and honest alcohol history remains an important part of evaluating liver disease.

Why Fatty Liver Disease Is a Growing Health Concern

MASLD has become one of the most common forms of chronic liver disease. Its increasing prevalence is closely connected to rising rates of insulin resistance, type 2 diabetes, obesity, metabolic syndrome, and abnormal blood lipids.

The condition matters for two major reasons. First, a proportion of people may progress from simple steatosis to MASH, fibrosis, cirrhosis, liver failure, or liver cancer. Fibrosis stage is one of the most important indicators of future liver-related risk.

Second, MASLD is a metabolic and cardiovascular health signal—not only a liver concern. People with fatty liver frequently have insulin resistance, abnormal lipids, high blood pressure, obesity, or type 2 diabetes. Cardiovascular risk assessment is therefore an important part of a comprehensive fatty liver evaluation.

Who Is More Likely to Develop MASLD?

Risk may increase when a person has one or more of the following:

  • Overweight, obesity, or increased waist circumference
  • Prediabetes, type 2 diabetes, or insulin resistance
  • High triglycerides or low HDL cholesterol
  • High LDL cholesterol or increased non-HDL cholesterol
  • High blood pressure
  • Metabolic syndrome
  • Polycystic ovary syndrome
  • Obstructive sleep apnea
  • A sedentary lifestyle
  • Diets high in sugar-sweetened beverages and highly refined carbohydrates
  • A family history or genetic susceptibility
  • Certain medications or medical conditions that can promote hepatic steatosis

MASLD can also occur in people whose body mass index is not in the overweight or obesity range. Body composition, visceral fat, ethnicity, genetics, diet, and metabolic health may influence risk independently of body weight.

Common Symptoms, Risk Factors, and Warning Signs

Most people with early MASLD do not have recognizable symptoms. When symptoms occur, they may be vague and may have many other possible explanations.

Symptom or Risk FactorWhat It May SuggestRelated Tests That May Provide Context
No symptoms but obesity, diabetes, or high triglyceridesIncreased metabolic risk despite feeling wellComprehensive Metabolic Panel, Hepatic Function Panel, Hemoglobin A1c, Glucose, Lipid Panel, and CBC with Differential and Platelets
Persistent fatigueA nonspecific symptom that may accompany metabolic, blood, thyroid, nutritional, or liver conditionsCBC with Differential and Platelets, Comprehensive Metabolic Panel, Thyroid Panel with TSH, Glucose, Hemoglobin A1c, and Ferritin, Iron and Total Iron Binding Capacity Panel
Mild discomfort in the upper-right abdomenPossible liver enlargement or another abdominal conditionHepatic Function Panel or Comprehensive Metabolic Panel; clinician-directed imaging may also be needed
Elevated ALT or ASTPossible liver-cell injury, although enzyme levels do not identify the causeALT Test, AST Test, GGT Test, Hepatitis B Test, Hepatitis C Antibody Test with Reflex to RNA, and Iron Studies
Elevated triglycerides or low HDL cholesterolPossible insulin resistance and increased cardiometabolic riskLipid Panel, Hemoglobin A1c, Fasting Glucose, Insulin Test, or Insulin Resistance Panel with Score
Type 2 diabetes or prediabetesHigher likelihood of MASLD and clinically important fibrosisHemoglobin A1c, Glucose Test, Comprehensive Metabolic Panel, CBC with Differential and Platelets, and FIB-4 assessment
Low platelet countMay occur with advanced fibrosis or portal hypertension but can have many other causesCBC with Differential and Platelets, Hepatic Function Panel, FIB-4, and clinician-directed fibrosis assessment
Jaundice, abdominal swelling, confusion, vomiting blood, or black stoolsPossible advanced or acutely serious liver diseaseSeek urgent medical assessment rather than relying on self-ordered testing

Safety note: Yellowing of the skin or eyes, confusion, severe abdominal swelling, vomiting blood, black or tarry stools, fainting, or sudden severe abdominal pain requires prompt medical attention.

Can You Have Fatty Liver With Normal Liver Enzymes?

Yes. ALT and AST may rise when liver cells are injured, but normal values do not rule out MASLD, MASH, or clinically important fibrosis.

Conversely, elevated liver enzymes do not establish that fatty liver is the cause. Viral hepatitis, alcohol exposure, medications, supplements, autoimmune disease, muscle injury, iron overload, and other conditions can also affect aminotransferase levels.

A complete assessment considers metabolic risk, laboratory trends, medical history, alcohol intake, medications, supplements, imaging, and—when appropriate—noninvasive fibrosis testing.

The Role of Lab Testing in Fatty Liver Evaluation

Blood testing may help patients and healthcare providers answer four practical questions.

1. Is There Evidence of Liver-Cell or Bile-Duct Injury?

An ALT Test, AST Test, Alkaline Phosphatase Test, Bilirubin Total Test, and GGT Test provide different types of information about liver and biliary health.

2. Are Metabolic Drivers Present?

A Glucose Test, Hemoglobin A1c Test, Insulin Test, Lipid Panel Test, and Apolipoprotein B Test can help identify metabolic patterns associated with MASLD.

3. Is Advanced Fibrosis More or Less Likely?

Age, AST, ALT, and the platelet count from a CBC with Differential and Platelets can be used to calculate FIB-4. An Albumin Test, Bilirubin Total Test, and Prothrombin Time with INR Test may provide additional context when advanced disease is suspected.

4. Could Another Condition Explain the Findings?

A Hepatitis B Test, Hepatitis C Antibody Test with Reflex to RNA, Ferritin Test, and Iron and Total Iron Binding Capacity Test may help investigate alternative or coexisting causes.

Lab tests cannot directly measure the percentage of liver fat, reliably distinguish simple steatosis from MASH, or stage fibrosis with complete certainty. Imaging and, in selected cases, liver biopsy may still be necessary.

Liver Injury and Function Tests

Test or BiomarkerWhat It MeasuresWhy It May MatterImportant Limitation
ALT TestAlanine aminotransferase, an enzyme found primarily in liver cellsMay increase when liver cells are irritated or injuredA normal result does not exclude MASLD, and an elevation is not specific to fatty liver
AST TestAspartate aminotransferase, an enzyme found in the liver, muscles, heart, and other tissuesUsed with ALT and included in the FIB-4 calculationMuscle injury and other non-liver conditions may raise AST
GGT TestGamma-glutamyl transferase, an enzyme associated with the liver and bile ductsMay add context to other liver or biliary abnormalitiesAlcohol, medications, and several liver conditions may influence the result
Alkaline Phosphatase TestAn enzyme produced by the bile ducts, bones, and other tissuesMay rise with bile-flow problems or certain liver conditionsAn elevated result may originate from bone rather than the liver
Bilirubin Total TestA pigment processed and excreted by the liverMay rise when bilirubin processing or bile flow is impairedHemolysis and benign inherited conditions may also affect bilirubin
Albumin TestAlbumin, a protein produced primarily by the liverLow levels may occur when liver protein production is impaired in advanced diseaseNutrition, inflammation, kidney loss, and other conditions can also affect albumin
Protein Total and Albumin TestTotal circulating protein and albuminProvides broader liver, nutritional, and protein-balance informationAbnormal results are not specific to MASLD
Prothrombin Time with INR TestHow long blood takes to clotMay reflect reduced production of clotting proteins in advanced liver diseaseAnticoagulants, vitamin K status, and other factors can alter the result

A Comprehensive Metabolic Panel includes several liver-related measurements along with glucose, kidney markers, electrolytes, and proteins. A Hepatic Function Panel provides a more focused review of liver enzymes, bilirubin, albumin, and total protein.

Metabolic and Cardiovascular Risk Tests

TestWhy It May Be Relevant
Fasting Glucose TestMeasures current blood glucose and may help identify impaired glucose regulation
Hemoglobin A1c TestEstimates average blood glucose exposure during approximately the previous two to three months
Insulin TestProvides information about circulating insulin and glucose regulation
C-Peptide TestProvides information about the body's insulin production
Insulin Resistance Panel with ScoreProvides a specialized assessment of insulin-resistance patterns when clinically appropriate
Lipid Panel TestMeasures total cholesterol, LDL cholesterol, HDL cholesterol, and triglycerides
Apolipoprotein B TestEstimates the number of atherogenic lipoprotein particles and may refine cardiovascular-risk assessment
High-Sensitivity C-Reactive Protein TestMeasures a nonspecific marker of systemic inflammation; it does not diagnose liver inflammation

The Nonalcoholic Fatty Liver Disease Base Assessment combines foundational liver and metabolic biomarkers that may help patients evaluate patterns associated with fatty liver risk.

Fibrosis-Risk Information

CBC with Differential and Platelets: Platelets may decrease as advanced liver fibrosis and portal hypertension develop, although a low platelet count can have many unrelated causes.

FIB-4: FIB-4 is calculated from age, AST, ALT, and the platelet count from a CBC with Differential and Platelets. It is widely used as an initial noninvasive tool to estimate the probability of advanced fibrosis.

Commonly used adult interpretation categories include:

  • Below 1.3: Lower probability of advanced fibrosis in many adults
  • 1.3 to 2.67: Further risk assessment may be appropriate
  • Above 2.67: Higher probability of advanced fibrosis that generally warrants clinical follow-up

Age affects interpretation. FIB-4 is less reliable in adults younger than 35, and a higher lower-risk threshold is often used in adults older than 65. FIB-4 should not be treated as a definitive diagnosis. People with obesity or type 2 diabetes may occasionally have meaningful fibrosis despite a lower score.

When FIB-4 or the overall clinical picture raises concern, a healthcare provider may recommend vibration-controlled transient elastography, the Enhanced Liver Fibrosis test, magnetic resonance elastography, or specialist evaluation.

Tests That May Help Evaluate Other Causes

Depending on the medical history and initial results, additional testing may include:

These tests are not required for everyone. Selection should be based on personal risk factors, symptoms, family history, medical history, and existing results.

1. Essential Baseline Assessment

A focused baseline may include:

This level may be appropriate for someone with metabolic risk factors, previously elevated liver enzymes, or an incidental imaging report describing hepatic steatosis. The Nonalcoholic Fatty Liver Disease Base Assessment provides a convenient bundled option for foundational testing.

2. Metabolic and Fibrosis-Risk Assessment

Additional testing may include:

The Nonalcoholic Fatty Liver Disease Advanced Assessment provides a broader evaluation of liver, glucose, insulin-resistance, lipid, and related metabolic biomarkers. Patients should review the current panel contents and preparation instructions before ordering.

3. Clinician-Directed Secondary Assessment

A healthcare provider may recommend:

  • Liver ultrasound
  • Vibration-controlled transient elastography, often called FibroScan
  • Enhanced Liver Fibrosis testing
  • MRI-based liver-fat or liver-stiffness measurement
  • Hepatology or gastroenterology referral
  • Liver biopsy when noninvasive findings are unclear or the diagnosis remains uncertain

Not everyone needs advanced imaging or a liver biopsy. A staged approach can help reduce unnecessary testing while identifying people who may require closer assessment.

4. Follow-Up and Monitoring

Follow-up monitoring may focus on:

The timing of repeat testing depends on the initial results, metabolic risk, medications, treatment plan, and clinician recommendations.

How to Understand Your Lab Results

Reference Ranges Are Not Diagnostic Cutoffs

A reference range represents values found in a laboratory's comparison population. A result outside the range does not automatically mean liver disease, and a result within the range does not guarantee that the liver is free of fat, inflammation, or fibrosis.

Look at Patterns, Not One Number

A healthcare provider may review:

Results May Vary

Laboratory values may be influenced by:

  • Fasting status
  • Hydration
  • Recent strenuous exercise
  • Acute illness
  • Alcohol consumption
  • Prescription medications
  • Nonprescription medicines
  • Vitamins, herbs, and supplements
  • Pregnancy
  • Age and sex
  • Laboratory methodology

Do not stop or change medications or supplements solely because of an abnormal result. Review possible contributors with the prescribing or treating healthcare professional.

How Ulta Lab Tests Helps

Ulta Lab Tests allows patients to order many blood tests directly online where available. Relevant options include individual liver and metabolic tests, the Nonalcoholic Fatty Liver Disease Base Assessment, and the Nonalcoholic Fatty Liver Disease Advanced Assessment.

Testing is performed through established laboratory networks such as Quest Diagnostics where applicable. Patients can review transparent pricing before ordering, no insurance is required, and eligible HSA or FSA payment may be available where accepted. Results are delivered securely online.

Direct-access testing can make it easier to establish a baseline, monitor previously discussed biomarkers, and prepare for a more productive healthcare visit. It does not replace professional diagnosis, imaging, treatment, or specialist care.

How to Prepare for Fatty Liver Blood Testing

  • Review the preparation instructions for every ordered test or panel.
  • Confirm whether fasting is required. A Lipid Panel Test, Glucose Test, Insulin Test, or specialized metabolic panel may have fasting instructions.
  • Maintain normal hydration unless instructed otherwise.
  • Avoid unusually strenuous exercise shortly before testing because it can affect AST and other biomarkers.
  • Do not change medications or supplements without guidance from a healthcare professional.
  • Bring identification and the required laboratory order or requisition.
  • Record current medications, supplements, recent illnesses, alcohol intake, and prior laboratory results for discussion with your provider.

Completing repeat testing under similar conditions can make laboratory trends easier to interpret.

Questions to Ask Your Healthcare Provider

  • Do my results suggest liver-cell injury, metabolic risk, or both?
  • Could a medication, supplement, alcohol exposure, or another condition explain my results?
  • Can my age, AST, ALT, and platelet count be used to calculate FIB-4?
  • Would ultrasound or transient elastography provide useful additional information?
  • Should I have a Hepatitis B Test, Hepatitis C Test, or Iron Studies Panel?
  • How often should my liver enzymes, platelets, glucose, and lipids be repeated?
  • Do my cardiovascular and diabetes risks need additional attention?
  • Should I see a gastroenterologist or hepatologist?
  • Are my current medicines appropriate for my liver and metabolic health?
  • Which symptoms should prompt urgent medical care?

Frequently Asked Questions

What blood tests are used for nonalcoholic fatty liver disease?

Common tests include an ALT Test, AST Test, Alkaline Phosphatase Test, GGT Test, Bilirubin Total Test, Albumin Test, Glucose Test, Hemoglobin A1c Test, Lipid Panel Test, and CBC with Differential and Platelets. No single blood test independently diagnoses or stages MASLD.

Is NAFLD the same as MASLD?

MASLD is the newer name for the condition previously called NAFLD. The updated term emphasizes the relationship between liver fat and cardiometabolic risk factors. NASH, the inflammatory form of the disease, is now called MASH. Older terminology remains common in medical records, research, and patient searches, so both sets of terms may appear.

Can a blood test confirm fatty liver?

Blood tests can identify liver abnormalities and metabolic risk factors, but they cannot directly confirm the amount of liver fat. Imaging such as ultrasound, transient elastography, CT, or MRI may identify hepatic steatosis. A liver biopsy is sometimes used when the diagnosis, inflammation, or fibrosis stage remains uncertain, but it is not required for most patients.

Can I have fatty liver if my ALT and AST are normal?

Yes. Normal ALT and AST levels do not completely exclude MASLD, MASH, or fibrosis. Results should be considered with diabetes status, body composition, triglycerides, platelet count, imaging, medications, alcohol exposure, and other risk factors.

What is the FIB-4 score?

FIB-4 is a noninvasive fibrosis-risk calculation that uses age, AST, ALT, and the platelet count from a CBC with Differential and Platelets. It helps identify people who may have a lower or higher probability of advanced liver fibrosis. It does not directly measure scar tissue and should not be used as a stand-alone diagnosis.

Does a high ALT mean I have fatty liver?

No. A high result on an ALT Test may indicate liver-cell injury, but it does not identify the cause. Fatty liver is one possibility. Viral hepatitis, alcohol-related injury, medication or supplement effects, autoimmune conditions, and other liver disorders may also raise ALT.

Why are A1c, glucose, insulin, and lipids included in fatty liver testing?

MASLD is closely connected to insulin resistance and cardiometabolic dysfunction. A Hemoglobin A1c Test and Glucose Test evaluate blood-sugar regulation. An Insulin Test may provide additional metabolic context. A Lipid Panel Test evaluates triglycerides, HDL cholesterol, LDL cholesterol, and other cardiovascular-risk markers.

Can fatty liver improve?

Liver fat and inflammation may improve when the metabolic factors contributing to MASLD are addressed. Weight management, physical activity, glucose control, lipid management, and treatment of related health conditions may be important. The appropriate plan should be individualized with a qualified healthcare professional.

Are there medications for MASH?

Prescription treatments are available for certain adults with MASH and moderate-to-advanced fibrosis. These treatments are intended for specific patients and require clinical evaluation, prescription, monitoring, and consideration of risks and contraindications. Laboratory testing alone cannot determine whether a medication is appropriate.

When should I repeat fatty liver blood tests?

Repeat timing depends on the initial results, metabolic risk, fibrosis assessment, medications, and care plan. Some people may need follow-up testing within several months, while lower-risk patients may be monitored less frequently. A healthcare provider can recommend an appropriate interval based on individual circumstances.

Can I order fatty liver blood tests without a doctor?

Ulta Lab Tests allows consumers to order many relevant liver and metabolic blood tests directly online where available. Options include individual tests, the Nonalcoholic Fatty Liver Disease Base Assessment, and the Nonalcoholic Fatty Liver Disease Advanced Assessment. Direct ordering provides information for discussion with a healthcare professional but does not replace diagnosis, imaging, treatment, or specialist evaluation.

Conclusion

Nonalcoholic fatty liver disease—now commonly called metabolic dysfunction-associated steatotic liver disease—is a growing health concern because it is common, often silent, and closely connected to diabetes, insulin resistance, abnormal lipids, cardiovascular disease, and obesity.

Blood tests cannot diagnose every stage of MASLD on their own, but they can reveal liver injury, metabolic risk, possible alternative causes, and information used to estimate fibrosis risk. Reviewing ALT, AST, GGT, bilirubin, albumin, platelets, glucose, Hemoglobin A1c, insulin, and lipids together creates a more useful picture than focusing on a single result.

Ulta Lab Tests provides convenient access to individual liver and metabolic tests as well as the Nonalcoholic Fatty Liver Disease Base Assessment and Nonalcoholic Fatty Liver Disease Advanced Assessment. Explore the available testing options and review your results with a qualified healthcare provider who can determine whether additional evaluation, imaging, monitoring, or treatment is appropriate.

References

  1. American Association for the Study of Liver Diseases: Clinical Assessment and Management of MASLD
  2. American Association for the Study of Liver Diseases: Changes in Fatty Liver Nomenclature
  3. American Association for the Study of Liver Diseases: Noninvasive Assessment of Patients With MASLD
  4. National Institute of Diabetes and Digestive and Kidney Diseases: Definition and Facts of NAFLD and NASH
  5. National Institute of Diabetes and Digestive and Kidney Diseases: Diagnosis of NAFLD and NASH
  6. National Institute of Diabetes and Digestive and Kidney Diseases: Treatment for NAFLD and NASH
  7. EASL–EASD–EASO Clinical Practice Guidelines on the Management of MASLD
  8. U.S. Food and Drug Administration: Approval of Resmetirom for MASH With Fibrosis
  9. U.S. Food and Drug Administration: Approval of Semaglutide for MASH
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Recommended Lab Tests

Fatty Liver Assessment Panels

Liver Injury and Liver Function Tests

Blood Count and Fibrosis-Risk Components

FIB-4 note: FIB-4 is a calculated fibrosis-risk score based on age, AST, ALT, and platelet count. It is not a separate blood test product.

Glucose Regulation and Insulin Resistance

Lipids and Cardiovascular Risk

Iron Status and Iron-Overload Evaluation

Viral Hepatitis Testing

Additional Tests for Alternative or Contributing Causes

These tests may be considered selectively based on medical history, symptoms, initial laboratory findings, and healthcare-provider guidance.

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