Loss of imprinting of a paternally expressed transcript, with antisense orientation to K V LQT1, occurs frequently in Beckwith–Wiedemann syndrome and is independent of insulin-like growth factor II imprinting
10.1073/pnas.96.9.5203
Crossref journal-article
Proceedings of the National Academy of Sciences
Proceedings of the National Academy of Sciences (341)
Abstract

Genomic imprinting plays a fundamental role in cancer and some hereditary diseases, including Beckwith–Wiedemann syndrome (BWS), a disorder of prenatal overgrowth and predisposition to embryonal malignancies such as Wilms tumor. We have previously shown that the K V LQT1 gene on chromosomal band 11p15 is imprinted, with expression of the maternal allele, and that the maternal allele is disrupted in rare BWS patients with balanced germ-line chromosomal rearrangements. We now show that an antisense orientation transcript within K V LQT1, termed LIT1 (long QT intronic transcript 1) is expressed normally from the paternal allele, from which K V LQT1 transcription is silent, and that in the majority of patients with BWS, LIT1 is abnormally expressed from both the paternal and maternal alleles. Eight of sixteen informative BWS patients (50%) showed biallelic expression, i.e., loss of imprinting (LOI) of LIT1. Similarly, 21 of 36 (58%) BWS patients showed loss of maternal allele-specific methylation of a CpG island upstream of LIT1. Surprisingly, LOI of LIT1 was not linked to LOI of insulin-like growth factor II (IGF2), which was found in 2 of 10 (20%) BWS patients, even though LOI of IGF2 occurs frequently in Wilms and other tumors, and in some patients with BWS. Thus, LOI of LIT1 is the most common genetic alteration in BWS. We propose that 11p15 harbors two imprinted gene domains—a more centromeric domain including K V LQT1 and p57 KIP2 , alterations in which are more common in BWS, and a more telomeric domain including IGF2, alterations in which are more common in cancer.

Bibliography

Lee, M. P., DeBaun, M. R., Mitsuya, K., Galonek, H. L., Brandenburg, S., Oshimura, M., & Feinberg, A. P. (1999). Loss of imprinting of a paternally expressed transcript, with antisense orientation to K V LQT1, occurs frequently in Beckwith–Wiedemann syndrome and is independent of insulin-like growth factor II imprinting. Proceedings of the National Academy of Sciences, 96(9), 5203–5208.

Authors 7
  1. Maxwell P. Lee (first)
  2. Michael R. DeBaun (additional)
  3. Kohzoh Mitsuya (additional)
  4. Heidi L. Galonek (additional)
  5. Sheri Brandenburg (additional)
  6. Mitsuo Oshimura (additional)
  7. Andrew P. Feinberg (additional)
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Dates
Type When
Created 23 years, 1 month ago (July 26, 2002, 10:43 a.m.)
Deposited 3 years, 4 months ago (April 13, 2022, 5:53 p.m.)
Indexed 4 weeks ago (Aug. 5, 2025, 8:35 a.m.)
Issued 26 years, 4 months ago (April 27, 1999)
Published 26 years, 4 months ago (April 27, 1999)
Published Online 26 years, 4 months ago (April 27, 1999)
Published Print 26 years, 4 months ago (April 27, 1999)
Funders 0

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@article{Lee_1999, title={Loss of imprinting of a paternally expressed transcript, with antisense orientation to K V LQT1, occurs frequently in Beckwith–Wiedemann syndrome and is independent of insulin-like growth factor II imprinting}, volume={96}, ISSN={1091-6490}, url={http://dx.doi.org/10.1073/pnas.96.9.5203}, DOI={10.1073/pnas.96.9.5203}, number={9}, journal={Proceedings of the National Academy of Sciences}, publisher={Proceedings of the National Academy of Sciences}, author={Lee, Maxwell P. and DeBaun, Michael R. and Mitsuya, Kohzoh and Galonek, Heidi L. and Brandenburg, Sheri and Oshimura, Mitsuo and Feinberg, Andrew P.}, year={1999}, month=apr, pages={5203–5208} }