Liver Cancer in Tyrosinemia Type 1

Willem G. van Ginkel; Jan P. Pennings; Francjan J. van Spronsen

doi:10.1007/978-3-319-55780-9_9

Liver Cancer in Tyrosinemia Type 1

Willem G. van Ginkel, Jan P. Pennings, Francjan J. van Spronsen^*

^*Corresponding author for this work

Research output: Chapter in Book/Report/Conference proceeding › Chapter › Academic › peer-review

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Abstract

Hereditary Tyrosinemia type I (HT1) is clinically mainly characterised by severe liver disease. Most patients present in their first months of life with liver failure, but others can present later with issues of compensated cirrhosis, renal tubulopathy or acute intermittent porphyria. If patients survive the acute phase with liver failure or if they present later with compensated cirrhosis, they often develop hepatocellular carcinoma early but also later in life. The course of the disease changed after the introduction of 2-(2 nitro-4-3 trifluoro-methylbenzoyl)-1,3-cyclohexanedione (NTBC), which blocks the tyrosine degradation pathway at an earlier step. Therefore, the toxic products did not accumulate anymore and all clinical problems resolved. However, the risk (although clearly decreased) for developing liver cancer remained, especially if NTBC treatment is initiated late, a slow decrease of the tumor marker alpha-fetoprotein is seen or if the alpha-fetoprotein concentrations remain just above the normal range. A rise of alpha-fetoprotein in these HT1 patients is more or less pathognomonic for liver cancer. Although hepatoblastoma development occurs in HT1 patients, most HT1 patients develop hepatocellular carcinoma (HCC) or a mixed type of carcinoma consisting of HCC and hepatoblastoma. Due to the small risk of liver cancer development, screening for liver cancer (especially HCC) is still recommended in HT1 patients using regular measures of alpha-fetoprotein and imaging. Ultrasound is mostly the modality of choice for surveillance, because it is widely available, it does not use radiation and is noninvasive. When a suspicious lesion is present, the higher sensitivity of MRI could be used for characterization and staging of lesions. At this moment, no HCC development in pre-symptomatically treated patients is reported. These different situations could possibly indicate that NTBC can prevent the start of the development of HCC when initiated early, but can't stop the development of HCC if it is prescribed at a later stage, stressing the importance of early diagnosis.

Original language	English
Title of host publication	HEREDITARY TYROSINEMIA: PATHOGENESIS, SCREENING AND MANAGEMENT
Editors	RM Tanguay
Publisher	Springer International Publishing AG
Chapter	9
Pages	101-109
Number of pages	9
ISBN (Electronic)	978-3-319-55780-9
ISBN (Print)	978-3-319-55779-3
DOIs	https://doi.org/10.1007/978-3-319-55780-9_9
Publication status	Published - 2017

Publication series

Name	Advances in Experimental Medicine and Biology
Publisher	SPRINGER INTERNATIONAL PUBLISHING AG
Volume	959
ISSN (Print)	0065-2598

Keywords

Tyrosinemia
Liver cancer
Hepatocellular carcinoma
HCC
AFP
Ultrasound
MRI
RADIOLOGIC-PATHOLOGICAL CORRELATION
HEREDITARY TYROSINEMIA
HEPATOCELLULAR-CARCINOMA
ALPHA-FETOPROTEIN
CHRONIC FORM
TRANSPLANTATION
NTBC
ABNORMALITIES
DIAGNOSIS
CIRRHOSIS

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@inbook{69eabb8541114d6cbd56bd8bbea24af0,

title = "Liver Cancer in Tyrosinemia Type 1",

abstract = "Hereditary Tyrosinemia type I (HT1) is clinically mainly characterised by severe liver disease. Most patients present in their first months of life with liver failure, but others can present later with issues of compensated cirrhosis, renal tubulopathy or acute intermittent porphyria. If patients survive the acute phase with liver failure or if they present later with compensated cirrhosis, they often develop hepatocellular carcinoma early but also later in life. The course of the disease changed after the introduction of 2-(2 nitro-4-3 trifluoro-methylbenzoyl)-1,3-cyclohexanedione (NTBC), which blocks the tyrosine degradation pathway at an earlier step. Therefore, the toxic products did not accumulate anymore and all clinical problems resolved. However, the risk (although clearly decreased) for developing liver cancer remained, especially if NTBC treatment is initiated late, a slow decrease of the tumor marker alpha-fetoprotein is seen or if the alpha-fetoprotein concentrations remain just above the normal range. A rise of alpha-fetoprotein in these HT1 patients is more or less pathognomonic for liver cancer. Although hepatoblastoma development occurs in HT1 patients, most HT1 patients develop hepatocellular carcinoma (HCC) or a mixed type of carcinoma consisting of HCC and hepatoblastoma. Due to the small risk of liver cancer development, screening for liver cancer (especially HCC) is still recommended in HT1 patients using regular measures of alpha-fetoprotein and imaging. Ultrasound is mostly the modality of choice for surveillance, because it is widely available, it does not use radiation and is noninvasive. When a suspicious lesion is present, the higher sensitivity of MRI could be used for characterization and staging of lesions. At this moment, no HCC development in pre-symptomatically treated patients is reported. These different situations could possibly indicate that NTBC can prevent the start of the development of HCC when initiated early, but can't stop the development of HCC if it is prescribed at a later stage, stressing the importance of early diagnosis.",

keywords = "Tyrosinemia, Liver cancer, Hepatocellular carcinoma, HCC, AFP, Ultrasound, MRI, RADIOLOGIC-PATHOLOGICAL CORRELATION, HEREDITARY TYROSINEMIA, HEPATOCELLULAR-CARCINOMA, ALPHA-FETOPROTEIN, CHRONIC FORM, TRANSPLANTATION, NTBC, ABNORMALITIES, DIAGNOSIS, CIRRHOSIS",

author = "{van Ginkel}, {Willem G.} and Pennings, {Jan P.} and {van Spronsen}, {Francjan J.}",

year = "2017",

doi = "10.1007/978-3-319-55780-9_9",

language = "English",

isbn = "978-3-319-55779-3",

series = "Advances in Experimental Medicine and Biology",

publisher = "Springer International Publishing AG",

pages = "101--109",

editor = "RM Tanguay",

booktitle = "HEREDITARY TYROSINEMIA: PATHOGENESIS, SCREENING AND MANAGEMENT",

}

Liver Cancer in Tyrosinemia Type 1. / van Ginkel, Willem G.; Pennings, Jan P.; van Spronsen, Francjan J.
HEREDITARY TYROSINEMIA: PATHOGENESIS, SCREENING AND MANAGEMENT. ed. / RM Tanguay. Springer International Publishing AG, 2017. p. 101-109 (Advances in Experimental Medicine and Biology; Vol. 959).

Research output: Chapter in Book/Report/Conference proceeding › Chapter › Academic › peer-review

TY - CHAP

T1 - Liver Cancer in Tyrosinemia Type 1

AU - van Ginkel, Willem G.

AU - Pennings, Jan P.

AU - van Spronsen, Francjan J.

PY - 2017

Y1 - 2017

N2 - Hereditary Tyrosinemia type I (HT1) is clinically mainly characterised by severe liver disease. Most patients present in their first months of life with liver failure, but others can present later with issues of compensated cirrhosis, renal tubulopathy or acute intermittent porphyria. If patients survive the acute phase with liver failure or if they present later with compensated cirrhosis, they often develop hepatocellular carcinoma early but also later in life. The course of the disease changed after the introduction of 2-(2 nitro-4-3 trifluoro-methylbenzoyl)-1,3-cyclohexanedione (NTBC), which blocks the tyrosine degradation pathway at an earlier step. Therefore, the toxic products did not accumulate anymore and all clinical problems resolved. However, the risk (although clearly decreased) for developing liver cancer remained, especially if NTBC treatment is initiated late, a slow decrease of the tumor marker alpha-fetoprotein is seen or if the alpha-fetoprotein concentrations remain just above the normal range. A rise of alpha-fetoprotein in these HT1 patients is more or less pathognomonic for liver cancer. Although hepatoblastoma development occurs in HT1 patients, most HT1 patients develop hepatocellular carcinoma (HCC) or a mixed type of carcinoma consisting of HCC and hepatoblastoma. Due to the small risk of liver cancer development, screening for liver cancer (especially HCC) is still recommended in HT1 patients using regular measures of alpha-fetoprotein and imaging. Ultrasound is mostly the modality of choice for surveillance, because it is widely available, it does not use radiation and is noninvasive. When a suspicious lesion is present, the higher sensitivity of MRI could be used for characterization and staging of lesions. At this moment, no HCC development in pre-symptomatically treated patients is reported. These different situations could possibly indicate that NTBC can prevent the start of the development of HCC when initiated early, but can't stop the development of HCC if it is prescribed at a later stage, stressing the importance of early diagnosis.

AB - Hereditary Tyrosinemia type I (HT1) is clinically mainly characterised by severe liver disease. Most patients present in their first months of life with liver failure, but others can present later with issues of compensated cirrhosis, renal tubulopathy or acute intermittent porphyria. If patients survive the acute phase with liver failure or if they present later with compensated cirrhosis, they often develop hepatocellular carcinoma early but also later in life. The course of the disease changed after the introduction of 2-(2 nitro-4-3 trifluoro-methylbenzoyl)-1,3-cyclohexanedione (NTBC), which blocks the tyrosine degradation pathway at an earlier step. Therefore, the toxic products did not accumulate anymore and all clinical problems resolved. However, the risk (although clearly decreased) for developing liver cancer remained, especially if NTBC treatment is initiated late, a slow decrease of the tumor marker alpha-fetoprotein is seen or if the alpha-fetoprotein concentrations remain just above the normal range. A rise of alpha-fetoprotein in these HT1 patients is more or less pathognomonic for liver cancer. Although hepatoblastoma development occurs in HT1 patients, most HT1 patients develop hepatocellular carcinoma (HCC) or a mixed type of carcinoma consisting of HCC and hepatoblastoma. Due to the small risk of liver cancer development, screening for liver cancer (especially HCC) is still recommended in HT1 patients using regular measures of alpha-fetoprotein and imaging. Ultrasound is mostly the modality of choice for surveillance, because it is widely available, it does not use radiation and is noninvasive. When a suspicious lesion is present, the higher sensitivity of MRI could be used for characterization and staging of lesions. At this moment, no HCC development in pre-symptomatically treated patients is reported. These different situations could possibly indicate that NTBC can prevent the start of the development of HCC when initiated early, but can't stop the development of HCC if it is prescribed at a later stage, stressing the importance of early diagnosis.

KW - Tyrosinemia

KW - Liver cancer

KW - Hepatocellular carcinoma

KW - HCC

KW - AFP

KW - Ultrasound

KW - MRI

KW - RADIOLOGIC-PATHOLOGICAL CORRELATION

KW - HEREDITARY TYROSINEMIA

KW - HEPATOCELLULAR-CARCINOMA

KW - ALPHA-FETOPROTEIN

KW - CHRONIC FORM

KW - TRANSPLANTATION

KW - NTBC

KW - ABNORMALITIES

KW - DIAGNOSIS

KW - CIRRHOSIS

U2 - 10.1007/978-3-319-55780-9_9

DO - 10.1007/978-3-319-55780-9_9

M3 - Chapter

SN - 978-3-319-55779-3

T3 - Advances in Experimental Medicine and Biology

SP - 101

EP - 109

BT - HEREDITARY TYROSINEMIA: PATHOGENESIS, SCREENING AND MANAGEMENT

A2 - Tanguay, RM

PB - Springer International Publishing AG

ER -

Liver Cancer in Tyrosinemia Type 1

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