AIM: Although liver cirrhosis is a predisposing factor for hepatocellular carcinoma (HCC), relatively few reports are available on HCC in primary biliary cirrhosis. High plasma nociceptin (N/OFQ) level has been shown in Wilson disease and in patients with acute and chronic pain. 

METHODS: We report a follow-up case of HCC, which developed in a patient with primary biliary cirrhosis. The tumor appeared 18 years after the diagnosis of PBC and led to death within two years. Alfa fetoprotein and serum nociceptin levels were monitored before and during the development of HCC. Nociceptin content was also measured in the tumor tissue. 

RESULTS: The importance and the curiosity of the presented case was the novel finding of the progressive elevation of plasma nociceptin level up to 17-fold (172 pg/mL) above the baseline (9.2 +/- 1.8 pg/mL) parallel with the elevation of alpha fetoprotein (from 13 ng/mL up to 3 480 ng/mL) during tumor development. Nociceptin content was more than 15-fold higher in the neoplastic tissue (0.16 pg/mg) than that in the tumor-free liver tissue samples (0.01 pg/mg) taken during the autopsy. 

CONCLUSION: Results are in concordance with our previous observation that a very high plasma nociceptin level may be considered as an indicator for hepatocellular carcinoma

Folhoffer, Anikó

Halász, Judit

Hantos, Mónika Beatrix

Horváth, Andrea

Illyés, György

Lakatos, Péter László

Schaff, Zsuzsa

Szalay, Ferenc

Tekes, Kornélia

World Journal of Gastroenterology

English

PubMed

Andrea Horvath

Aniko Folhoffer

Peter Laszlo Lakatos

Judit Halász

Gyorgy Illyés

Zsuzsa Schaff

Monika Beatrix Hantos

Kornelia Tekes

Ferenc Szalay

Crossref

Rising plasma nociceptin level during development of HCC: A case report

Repository of the Academy's Library

P.O.Box 2345, Beijing 100023,China                                                                                                                                                                  World J Gastroenterol  2004;10(1):152-154Fax: +86-10-85381893                                                                                                                                                                                                                                 World Journal of GastroenterologyE-mail: wjg@wjgnet.com     www.wjgnet.com                                                                                                                                   Copyright © 2004 by The WJG Press ISSN 1007-9327• CASE REPORT •Rising plasma nociceptin level during development of HCC: A casereportAndrea Horvath, Aniko Folhoffer, Peter Laszlo Lakatos, Judit Halász, Gyorgy Illyés, Zsuzsa Schaff, Monika BeatrixHantos, Kornelia Tekes, Ferenc SzalayAndrea Horvath, Aniko Folhoffer, Peter Laszlo Lakatos, FerencSzalay, 1st Department of Medicine of Semmelweis University,Budapest, HungaryJudit Halász, Gyorgy Illyés, Zsuzsa Schaff, 2nd Department ofPathology of Semmelweis University, Budapest, HungaryKornelia Tekes, Department of Pharmacodynamics of SemmelweisUniversity, Budapest, HungaryMonika Beatrix Hantos, Neurochemical Research Unit of HungarianAcademy of Sciences, Budapest, HungaryCorrespondence to: Szalay Ferenc, MD, PhD, 1st Department ofMedicine, Semmelweis University, Korányi St. 2/A, H-1083Budapest, Hungary.  szalay@bel1.sote.huTelephone: +36-1-210-1007    Fax: +36-1-210-1007Received: 2003-09-23    Accepted: 2003-11-16AbstractAIM: Although liver cirrhosis is a predisposing factor forhepatocellular carcinoma (HCC), relatively few reports areavailable on HCC in primary biliary cirrhosis. High plasmanociceptin (N/OFQ) level has been shown in Wilson diseaseand in patients with acute and chronic pain.METHODS: We report a follow-up case of HCC, whichdeveloped in a patient with primary biliary cirrhosis. The tumorappeared 18 years after the diagnosis of PBC and led to deathwithin two years. Alfa fetoprotein and serum nociceptin levelswere monitored before and during the development of HCC.Nociceptin content was also measured in the tumor tissue.RESULTS: The importance and the curiosity of the presentedcase was the novel finding of the progressive elevation ofplasma nociceptin level up to 17-fold (172 pg/mL) above thebaseline (9.2±1.8 pg/mL), parallel with the elevation of alphafetoprotein (from 13 ng/mL up to 3 480 ng/mL) during tumordevelopment. Nociceptin content was more than 15-fold higherin the neoplastic tissue (0.16 pg/mg) than that in the tumor-free liver tissue samples (0.01 pg/mg) taken during the autopsy.CONCLUSION: Results are in concordance with our previousobservation that a very high plasma nociceptin level may beconsidered as an indicator for hepatocellular carcinoma.Horvath A, Folhoffer A, Lakatos PL, Halász J, Illyés G, Schaff Z,Hantos MB, Tekes K, Szalay F. Rising plasma nociceptin levelduring development of HCC: A case report. World J Gastroenterol2004; 10(1): 152-154http://www.wjgnet.com/1007-9327/10/152.aspINTRODUCTIONThe incidence of hepatocellular carcinoma (HCC) in primarybiliary cirrhosis (PBC) is reported to range from 0.5% to 4.2%,which is somewhat less frequent than that in liver cirrhosisfrom other etiologies[1,2]. However, recent reports have shownan increasing trend. The incidence of HCC was found higherin stage III/IV than in stage I/II patients[1,3,4].      Relatively few prospective and comprehensive studies areavailable on HCC in PBC, and the number of case reports isalso limited. Summarizing the data of the literature, 126 of6 188 PBC patients (2.0%) were found to have HCC. SinceHCC usually develops many years after the diagnosis of PBC,screening of HCC has clinical importance and offers best withhope for early detection. Serum AFP is a widely acceptedmarker of HCC[5]; however, using the conventional cut-offvalue of 500 ng/mL, it has a sensitivity of about 50% and aspecificity of more than 90% in detecting HCC in a patientwith coexisting liver disease[6]. The average survival of patientswith HCC improved in the last decades[7]. Female HCC patientsoften have a better prognosis than male patients[8]. Because ofthe lack of sensitive markers of malignant hepatic tumors, HCCis usually recognized in the advanced stage.     We reported a follow-up case of HCC in a PBC patient.The importance of this case is the novel finding of progressiveelevation in plasma nociceptin (N/OFQ, formerly named asorphanin FQ) up to 17-fold above the baseline, parallel withthe elevation of alpha fetoprotein (AFP) during tumordevelopment. Moreover, high nociceptin content was foundin the tumor tissue as well.    Nociceptin, a newly discovered neuropeptide of 17aminoacids, is the natural agonist of NOP receptor, earliernamed opioid receptor-like 1 (ORL1) receptor. N/OFQ is aneuropeptide that is endowed with pronociceptive activity invivo. Both the long and the short splice variants of the OP4receptor mRNA were isolated in rat liver[9]; however, there areno data about its physiological or pathophysiological role inliver function. To date only few clinical studies on nociceptinwere reported, and only one of them dealt with liver disease.      Findings of the presented case are in concordance with ourprevious observation that a high plasma NC level may be anindicator of HCC.CASE REPORTA 47-year-old woman was admitted for fatigue, itching,hepatomegaly, high alkaline phophatase and gamma-GT levels.Primary biliary cirrhosis was diagnosed based on the clinicalsymptoms, laboratory findings, AMA M2 positivity, normalUS and ERCP pictures. Liver biopsy revealed stage II/III. Therewas no family history of liver disease or autoimmune disease,and all other confounding risk factors including alcohol, HBVand HCV infections were excluded. The patient was a heavysmoker. The past surgical history was significant only for anappendectomy and two caesarean sections. Her menopausestarted at the age of 38. Bone mineral density was slightlybelow the normal range at the time of diagnosis of PBC.Ursodeoxycholic acid (Ursofalk) treatment, calcium andvitamin D supplementation were introduced.     Severe progression of osteoporosis was observed duringthe following years. Five years after the diagnosis of PBCsignificantly decreased bone mineral density was shown bothon the femoral neck (T-score: -5.12, Z score: -3.38) and on thelumbar vertebrae (T-score: -5.44, Z-score: -3.9). At the age of57 despite the calcium, vitamin-D supplementation, calcitoninand bisphophonate (Fosamax) treatment, the severe osteoporosisled to hip fracture and multiple vertebral collapses, which madethe patient lifelong disabled.      Progression of PBC to stage IV occured. She was monitoredby yearly US, by regular laboratory tests and AFP every 3-4months. For different reasons we collected blood samples forplasma nociceptin level determination as well. Sampling wasdone in conformity to accepted ethical standards and wasapproved by the regional ethical committee.     Hepatocellular carcinoma developed 18 years after thediagnosis of PBC. Regular follow-up US investigationsrevealed a focal lesion of 2.5 cm in diameter, which increasedrapidly in segment V of the liver. Fine needle biopsy findingsproved hepatocellular carcinoma. After the HCC diagnosis acontinuous and rapid increase in the size of the tumor, anelevation of ALP, GGT, plasma nociceptin and AFP levelsand clinical deterioration were observed.Figure 1  Serum alpha fetoprotein and plasma nociceptin lev-els before and during the development of hepatocellular carci-noma in the presented patient with primary biliary cirrhosis.Figure 2  Hepatocellular carcinoma in the presented patientwith primary biliary cirrhosis. A: Gross view of liver at autopsy.Grayish nodules of carcinoma protrude on the surface of thecirrhotic liver. Bar=1 cm. B: The focal red staining on the histo-logic picture of the hepatocellular carcinoma shows the immu-nohistochemical reaction of AFP. Original magnification 400×.     The AFP value had been within the normal range one yearbefore the tumor was detected (13 ng/mL), but it was elevatedat the time of the diagnosis of HCC (426 ng/mL) and rose up to3 480 ng/ml. The plasma nociceptin measured by radioimmunoassay125I-Nociceptin-kit, Phoenix Pharmaceuticals, Phoenix, CA,USA (10.6 pg/mL) was within the normal range (9.2±1.8 pg/mL)in the tumor-free stage, while progressive elevation was detectedduring the tumor development (15.8, 65.8, 103.7, 128.0,172.2 pg/mL), reaching the highest value before death (Figure1). Higher nociceptin content was measured in the tumor tissue(0.16 pg/mg) compared to the tumor-free liver tissue sample(0.01 pg/mg) taken during the autopsy. The patient refused anysurgical or other systemic or local tumor treatment. The size ofthe tumor increased up to 12 cm in diameter and involvedsegments V, VII, VIII and partly IV. No metastasis was detected,but necrosis developed in the central region of the tumor. Thepatient received supportive treatment, analgetics, and died oftumorous cachexia 19 months after the discovery of HCC. Theautopsy confirmed both PBC stage IV and HCC. Focal presenceof AFP was shown in the tumor by immunohistochemistry(Figures 2 A and B).      A nociceptin content in the HCC tissue (0.16 pg/mg) was15-fold higher than that in the tumor free liver tissue sample(0.01 pg/mg) taken during the autopsy.DISCUSSIONThe presented case is a further example of the occurrence ofHCC in PBC, and it supports previous observations that HCCusually develops in stage III/IV patients[3]. The tumor developed18 years after the diagnosis of PBC and led to the death of thepatient within two years. Furthermore, severe osteoporosis isa common disorder in PBC, although recently it is consideredas a non-specific complication[10,11 ]. In our patient the earlymenopause together with PBC resulted in many bone fracturescausing lifelong disability. The low serum osteocalcin levelindicated a low turnover osteoporosis. High serum osteoprotegerinand low RANKL have been reported in PBC[12], and we foundthe same alteration in this patient. Progression of bone loss wasdetected despite the serum osteoprotegerin was two-fold higherthan normal, which suggested that inflammatory process in theliver could also contribute to the elevation of osteoprotegerin.    This is the first follow-up case in which progressiveelevation of plasma nociceptin level was detected in parallelwith the elevation of AFP during tumor development, and highN/OFQ content was found in the tumor tissue.     Nociceptin is the endogenous agonist of a G-proteincoupled, naloxon insensitive opioid-like 1 receptor (ORL1)recently named as OP4. Although nociceptin is structurallyrelated to opioid peptides, especially to dynorphin A, it doesnot interact with m, d and k receptors. N/OFQ/OP4 system is anewly discovered peptide-based signalling pathway, involvedin the modulation of pain and cognition. Opioid antagonistswere successfully used for the treatment of pruritus in patientswith PBC[13]. These results together with the data that highplasma N/OFQ level has been reported in Wilson disease andin patients with chronic pain, led us to measure plasmanociceptin level in primary biliary cirrhosis[14]. Our motivationwas reinforced by an accidental observation that we foundextremely high N/OFQ in a Wilson patient with advanced HCC.     The nociceptin levels in blood samples collected in thepre-tumor stage and during the tumor development periodclearly showed that the elevation of N/OFQ was parallel withthat of AFP and the clinical deterioration. When the tumorwas first detected the N/OFQ level was 6-fold higher than thatin healthy controls (65.8 versus 9.2±1.8 pg/mL, n=29) and inother PBC patients without HCC (12.1±3.2pg/mL, n=21).When the tumor reached 11 cm the N/OFQ level was 17-foldAFP (ng/mL)4 0003 5003 0002 5002 0001 5001 0005000NC (pg/mL)200180160140120100806040200AFP      pg/mLNC       pg/mLUS: 2.5 cmfocal lesionUS: 11 cmfocal lesion10.200006.200102.200104.200112.200008.200110.200112.200102.200204.200206.200208.200210.200212.2002Time (month/year)ABHorvath A et al. Nociceptin in HCC            153higher than normal. Since N/OFQ content was 15-fold higherin tumor tissue than in tumor free parts of the liver, the questionarose whether nociceptin was produced by HCC tissue or itaccumulated in the tumor by passive binding or via increasednociceptin receptor expression.     Further research is needed to clarify the mechanism andclinical significance of the highly elevated N/OFQ level inHCC. Since N/OFQ transcripts are expressed in immunecells[15], the high N/OFQ level may also be an indicator ofaltered reaction of the body including immunological,cytokine and other mechanisms.     Elevated N/OFQ level might represent a compensatorymechanism in the N/OFQ/OP4 system to modulate painperception in the central nervous system. This mechanism couldexplain why some patients with a very high plasma N/OFQlevel did not have pain despite advanced stage of malignantliver tumor. It is remarkable that the N/OFQ was 3-fold higherin our patient than the highest values reported in patients withchronic pain without malignant disease[16].    In conclusion, the novel finding of this study is thatprogressive elevation of plasma nociceptin was detected inparallel with the elevation of AFP during tumor development,as well as high N/OFQ content was found in the tumor tissuein a PBC patient with hepatocellular carcinoma. This is inconcordance with our previous observation that high plasmaN/OFQ level might be considered as an indicator of HCC.REFERENCES1 Nakanuma Y, Terada T, Doishita K, Miwa A. Hepatocellular car-cinoma in primary biliary cirrhosis: an autopsy study. Hepatology1990; 11: 1010-10162 Krasner N, Johnson PJ, Portmann B, Watkinson G, MacsweenRNM, Williams R. Hepatocellular carcinoma in primary biliarycirrhosis. Gut 1979; 20: 255-2583 Jones D, Metcalf J, Collier J, Bassendine M, James O. Hepatocel-lular carcinoma in primary biliary cirrhosis and its impact onoutcomes. Hepatology 1997; 26: 1138-11424 Caballeria L, Pares A, Castells A, Gines A, Bru C, Rodes J. Hepa-tocellular carcinoma in primary biliary cirrhosis: similar incidenceto that in hepatitis C virus-related cirrhosis. Am J Gastroenterol2001; 96: 1160-11635 Nguyen MH, Keefe EB. Screening for hepatocellular carcinoma.J Clin Gastroenterol 2002; 35(5 Suppl 2): S86-916 Johnson PJ. The role of serum alpha-fetoprotein estimation inthe diagnosis and management of hepatocellular carcinoma. ClinLiver Dis 2001; 5: 145-1597 Tang ZY. Clinical research of hepatocellular carcinoma in the21st century. China Natl J Gastroenterol 1995; 1: 2-38 Qin LX, Tang ZY. The prognostic significance of clinical andpathological features in hepatocellular carcinoma. World JGastroenterol 2002; 8: 193-1999 Wang JB, Johnson PS, Imai Y, Persico AM, Ozenberger BA, EpplerCM, Uhl GR. cDNA cloning of an orphan opiate receptor genefamily member and its splice variant. FEBS Lett 1994; 348: 75-7910 Newton J, Francis R, Prince M, James O, Bassendine M, RawlingsD, Jones D. Osteoporosis in primary biliary cirrhosis revisited.Gut 2001; 49: 282-28711 Floreani A. Osteoporosis is not a specific complication of primarybiliary cirrhosis (PBC). Gut 2002; 50: 898; author reply 898-89912 Szalay F, Hegedus D, Lakatos PL, Tornai I, Bajnok E, Dunkel K,Lakatos P. High serum osteoprotegerin and low RANKL in pri-mary biliary cirrhosis. J Hepatol 2003; 38: 395-40013 Neuberger J, Jones EA. Liver transplantation for intractable pru-ritus is contraindicated before an adequate trial of opiate antago-nist therapy. Eur J Gastroenterol Hepatol 2001; 13: 1393-139414 Hantos MB, Szalay F, Lakatos PL, Hegedus D, Firneisz G,Reiczigel J, Torok T, Tekes K. Elevated plasma nociceptin levelin patients with Wilson disease. Brain Res Bull 2002; 58: 311-31315 Arjomand J, Cole S, Evans C. Novel orphanin FQ/nociceptintranscripts are expressed in human immune cells. J Neuroimmunol2002; 13: 1631-163316 Ko MH, Kim YH, Woo RS, Kim KW. Quantitive analysis ofnociceptin in blood of patients with acute and chronic pain.Neuroreport 2002; 13: 1361-1363Edited by Zhang JZ154                    ISSN 1007-9327      CN 14-1219/ R        World J Gastroenterol    January 1, 2004   Volume 10   Number 1

cDNA cloning of an orphan opiate receptor gene family member and its splice variant.

Clinical research of hepatocellular carcinoma

Elevated plasma nociceptin level in patients with Wilson disease.

Hepatocellular carcinoma in primary biliary cirrhosis and its impact on outcomes. Hepatology

Hepatocellular carcinoma in primary biliary cirrhosis: an autopsy study. Hepatology

Hepatocellular carcinoma in primary biliary cirrhosis: similar incidence to that in hepatitis C virus-related cirrhosis.

Hepatocellular carcinoma in primary biliary cirrhosis. Gut

High serum osteoprotegerin and low RANKL in primary biliary cirrhosis.

Liver transplantation for intractable pruritus is contraindicated before an adequate trial of opiate antagonist therapy.

Novel orphanin FQ/nociceptin transcripts are expressed in human immune cells.

Osteoporosis in primary biliary cirrhosis revisited. Gut

Osteoporosis is not a specific complication of primary biliary cirrhosis (PBC). Gut 2002; 50: 898; author reply

Quantitive analysis of nociceptin in blood of patients with acute and chronic pain. Neuroreport

Screening for hepatocellular carcinoma.

The prognostic significance of clinical and pathological features in hepatocellular carcinoma.

The role of serum alpha-fetoprotein estimation in the diagnosis and management of hepatocellular carcinoma. Clin Liver Dis

Rising plasma nociceptin level during development of HCC: A case report

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