Hepatocellular adenomas: Magnetic resonance imaging features as a function of molecular pathological classification

Laumonier, H.; Bioulac‐Sage, Paulette; Laurent, Césari; Zucman‐Rossi, Jessica; Balabaud, Charles; Trillaud, Hervé

doi:10.1002/hep.22417

Cited by 279 publications

(236 citation statements)

References 21 publications

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“…Autophagy defects lead to enhancement of oxidative stresses and promotion of inflammation and pyroptosis (Mizushima et al ., 1998; Liu et al ., 2012; Lamkanfi & Dixit, 2014). Sinusoidal dilatation is a type of vascular liver lesions previously reported to be associated with inflammatory hepatocellular adenoma (formerly known as telangiectatic focal nodular hyperplasia) (Laumonier et al ., 2008). It is characterized by widening of hepatic capillaries and may impair their contractile properties (Saadoun et al ., 2004).…”

Section: Discussionmentioning

confidence: 99%

Defects in MAP1S‐mediated autophagy cause reduction in mouse lifespans especially when fibronectin is overexpressed

Zou

Fei

et al. 2016

Aging Cell

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SummaryAutophagy is a cellular process that executes the turnover of dysfunctional organelles and misfolded or abnormally aggregated proteins. Microtubule‐associated protein MAP1S interacts with autophagy marker LC3 and positively regulates autophagy flux. LC3 binds with fibronectin mRNA and facilitates its translation. The synthesized fibronectin protein is exported to cell surface to initiate the assembly of fibronectin extracellular matrix. Fibronectin is degraded in lysosomes after it is engulfed into cytosol via endocytosis. Here, we show that defects in MAP1S‐mediated autophagy trigger oxidative stress, sinusoidal dilation, and lifespan reduction. Overexpression of LC3 in wild‐type mice increases the levels of fibronectin and γ‐H2 AX, a marker of DNA double‐strand breakage. LC3‐induced fibronectin is efficiently degraded in lysosomes to maintain a balance of fibronectin levels in wild‐type mice so that the mice live a normal term of lifespan. In the LC3 transgenic mice with MAP1S deleted, LC3 enhances the synthesis of fibronectin but the MAP1S depletion causes an impairment of the lysosomal degradation of fibronectin. The accumulation of fibronectin protein promotes liver fibrosis, induces an accumulation of cell population at the G0/G1 stage, and further intensifies oxidative stress and sinusoidal dilatation. The LC3‐induced overexpression of fibronectin imposes stresses on MAP1S‐deficient mice and dramatically reduces their lifespans. Therefore, MAP1S‐mediated autophagy plays an important role in maintaining mouse lifespan especially in the presence of extra amount of fibronectin.

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Section: Discussionmentioning

confidence: 99%

Defects in MAP1S‐mediated autophagy cause reduction in mouse lifespans especially when fibronectin is overexpressed

Zou

Fei

et al. 2016

Aging Cell

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“…These different subtypes show variable clinical behaviour, imaging findings, and natural history, and thus the options for treatment surveillance may vary (7). The MRI findings of different subtypes of hepatocellular adenomas have been reported by Laumonier et al (11). HNF-1alpha-mutated hepatocellular adenomas and inflammatory hepatocellular adenomas have been described to be associated with specific MRI patterns and related to diffuse fat distribution and to sinusoidal dilatation, respectively.…”

Section: Case Reportmentioning

confidence: 71%

“…After gadolinium-based contrast material administration moderate enhancement is noted in the arterial phase, with absence of persistent enhancement in the portal venous and delayed phases (7,11). A homogeneous signal drop-off on chemical shift images for the diagnosis of HNF-1alpha-mutated hepatocellular adenomas has been shown a sensitivity and specificity of 86% and 100% respectively (11). No specific MRI imaging features have been described for the diagnosis betacatenin-mutated hepatocellular adenomas.…”

Section: Discussionmentioning

confidence: 99%

“…With extracellular gadolinium-based contrast media strong arterial enhancement that may or may not persist on the portal venous and delayed phases can be seen. Beta-catenin-mutated hepatocellular adenomas may mimic hepatocellular carcinoma (7,11).…”

Section: Discussionmentioning

confidence: 99%

“…After intravenous administration of gadolinium-based contrast material intense enhancement during the arterial phase is seen, with persistent enhancement in the portal venous and delayed phases (7,11). A marked T2 hyperintensity together with delayed persistent enhancement for the diagnosis of inflammatory hepatocellular adenomas has been reported to correspond with a sensitivity of 85% and a specificity of 87% (11). HNF-1alpha-mutated hepatocellular adenomas are are isoinpatients (3).…”

Section: Case Reportmentioning

confidence: 99%

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Hepatic adenomatosis: MR Imaging Features

Kock

Smet

et al. 2014

Journal of the Belgian Society of Radiology

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Hepatic adenomatosis occurs predominantly in women during the 4 th and 5 th decades of life (1). Hepatic adenomatosis is rare, although its real frequency could be underestimated because many patients are asymptomatic. Hepatic adenomatosis is defined as the presence of multiple adenomas (arbitrarily > 10) involving both lobes of the liver. Patients with glycogen storage disease or with a history of steroid intake are not considered to have liver adenomatosis (1, 2).Although the exact aetiology of hepatic adenomatosis is still unclear, congenital or acquired hepatic vascular abnormalities, mutations of the hepatocyte nuclear factor 1alpha (HNF1A) gene, and non-alcoholic fatty liver disease have been proposed as potential causes for the development of hepatic adenomatosis (1, 2). Hepatocellular adenomas in patients with hepatic adenomatosis may be of the inflammatory, HNF-1alpha-mutated, or beta-catenin-mutated subtypes, and as a consequence may show variable imaging findings.We describe the magnetic resonance imaging (MRI) findings in a 39-year-old woman presenting with non-alcoholic fatty liver disease and hepatic adenomatosis characterized by the inflammatory subtype of hepatic adenomas. minimal or no signal drop-off on chemical shift sequences. On T1-weighted in-phase images, lesions were isointense or mildly hyperintense compared to liver parenchyma (Fig. 1). On fat suppressed T1-weighed images, due to liver steatosis, lesions were markedly hyperintense (Fig. 2). One lesion measuring 8 cm demonstrated an irregular central T1-and T2-weighted hypointense area. Case reportA 39-year-old female with unremarkable previous medical history was referred for MRI after detecting a large liver mass during routine ultrasound examination. Patient had taken oral contraceptives for 12 years. Physical examination showed slight overweight (body mass index 29). The laboratory evaluations and blood biochemistry profile showed elevated C-reactive protein (11,4 mg/dl; normal value < 0,5), alkaline phosphatase (417 U/L, normal values 27-126) and γ-glutamyltransferase (101 U/L, normal values 5-43) levels. Hepatitis B surface antigen, anti-hepatitis B surface antibody and anti-hepatitis C antibody were negative.Serum alpha-fetoprotein (AFP), carcinoembryonic antigen (CEA) and carbohydrate antigenic determinant (CA) 19-9 were normal. On MRI, liver parenchyma showed marked signal drop-off on T1-weighted out-ofphase images and corresponded to steatosis of the liver parenchyma. Multiple, approximately 14, well-delineated focal liver lesions with variable size (1-10 cm diameter) involving both liver lobes were noted. Lesions were diffusely hyperintense on T2-weighted images, with higher signal intensity in the periphery of the lesion (Fig. 1) We report a case with the inflammatory subtype of hepatic adenomatosis in a 39-year-old woman with liver steatosis. the magnetic resonance imaging features using extracellular gadolinium chelates and hepatocytetargeted contrast agents are described.

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Benign Tumors, Nodules, and Cystic Diseases of the Liver

Caldéraro

Zucman–Rossi

2017

Schiff's Diseases of the Liver

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Hepatocellular adenomas: Magnetic resonance imaging features as a function of molecular pathological classification

Cited by 279 publications

References 21 publications

Defects in MAP1S‐mediated autophagy cause reduction in mouse lifespans especially when fibronectin is overexpressed

Defects in MAP1S‐mediated autophagy cause reduction in mouse lifespans especially when fibronectin is overexpressed

Hepatic adenomatosis: MR Imaging Features

Benign Tumors, Nodules, and Cystic Diseases of the Liver

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