Loss of Heterozygosity on Chromosome 11p15.5 and Relapse in Hepatoblastomas

S. Chitragar; V. K. Iyer; S. Agarwala; S. D. Gupta; A. Sharma; M. N. Wari

doi:10.1055/s-0030-1267208

European Journal of Pediatric Surgery, Inhaltsverzeichnis

Eur J Pediatr Surg 2011; 21(1): 50-53
DOI: 10.1055/s-0030-1267208

Original Article

Loss of Heterozygosity on Chromosome 11p15.5 and Relapse in Hepatoblastomas

S. Chitragar¹ , V. K. Iyer¹ , S. Agarwala² , S. D. Gupta¹ , A. Sharma³ , M. N. Wari¹

¹All India Institute of Medical Sciences, Pathology, New Delhi, India
²All India Institute of Medical Sciences, Pediatric Surgery, New Delhi, India
³All India Institute of Medical Sciences, Anatomy, New Delhi, India

Abstract

Background: IGF2 is a tumor suppressor gene at locus 11p15. Many hepatoblastomas have loss of heterozygosity (LOH) at this locus. Earlier studies have not demonstrated any association between LOH and prognosis. Aim of the study was to evaluate the prognostic significance of LOH at 11p15.5 in hepatoblastomas.

Methods: DNA was isolated from normal liver and tumor tissue in 20 patients with hepatoblastoma. PCR was performed and cases were classified as LOH present, absent or non-informative. Patients’ follow-up data was analyzed using Fischer's exact test and Kaplan-Meier survival analysis for relapse-free survival (RFS) in relation to LOH. Ethical clearance was obtained from the institutional ethics board.

Results: All cases were informative for at least one microsatellite marker used. 4 of the 20 cases (20%) had LOH at 11p15.5. One patient died in the immediate postoperative period. 5 of 19 patients relapsed (26%). Of 4 patients who had LOH, 3 (75%) relapsed, the time to relapse being 7, 7 and 9 months, respectively. Of the 15 cases without LOH, 2 (13.3%) relapsed. 4 patients had mixed epithelial and mesenchymal histology; 3 of them had LOH. The 2 groups with and without LOH were well matched. The RFS for patients with LOH (n=4) was 13% (mean survival time [MST]: 8.7 months; 95CI 6.7–10.7), while the RFS for cases without LOH (n=15) was 75% (MST: 100.7 months; 95CI 74.5–126.8).

Conclusion: Mixed epithelial and mesenchymal histology is more frequently associated with LOH on chromosome 11p15.5 than pure epithelial histology. LOH on chromosome 11p15.5 is associated with a significantly increased incidence of relapse and a significantly shorter relapse-free survival in patients with hepatoblastoma. The risk of relapse is higher and the RFS lower both in standard-risk and high-risk patients with hepatoblastoma if they demonstrate the presence of LOH at 11p15.5.

Key words

loss of heterozygosity - relapse - hepatoblastoma

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References

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Correspondence

Dr. Sandeep Agarwala

All India Institute of Medical

Sciences

Department of Pediatric

Surgery

110029 New Delhi

India

Telefon: +91/11/265 93309

Fax: +91/11/265 88640

eMail: sandpagr@hotmail.com