Hostname: page-component-586b7cd67f-l7hp2 Total loading time: 0 Render date: 2024-11-22T21:22:40.788Z Has data issue: false hasContentIssue false

Absence of Pericentromeric Heterochromatin (9qh-) in a Patient with Bilateral Retinoblastoma

Published online by Cambridge University Press:  01 August 2014

T. A. Sivakumaran
Affiliation:
Division of Genetics, Department of Anatomy
S. Ghose
Affiliation:
Pediatric Ophthalmology Service, Dr. Rajendra Prasad Center for Ophthalmic Sciences, All India of Medical Sciences, New Delhi, India
H. Kumar
Affiliation:
Pediatric Ophthalmology Service, Dr. Rajendra Prasad Center for Ophthalmic Sciences, All India of Medical Sciences, New Delhi, India
U. Singha
Affiliation:
Pediatric Ophthalmology Service, Dr. Rajendra Prasad Center for Ophthalmic Sciences, All India of Medical Sciences, New Delhi, India
K. Kucheria*
Affiliation:
Division of Genetics, Department of Anatomy
*
Division of Genetics, Department of Anatomy, All India Institute of Medical Sciences, New Delhi 110 029, INDIAe-mail:, [email protected].

Abstract

Core share and HTML view are not available for this content. However, as you have access to this content, a full PDF is available via the ‘Save PDF’ action button.

The polymorphisms of constitutive heterochromatin regions, present on chromosomes 1, 9, 16 and Y, are inherited in a Mendelian fashion. The C-band heteromorphism has been reported to be associated with various types of cancer. Heterochromatin is considered to play a role in protecting genome against the mutagens. Changes in the quantity and proportion of the different types of satellite DNA might increase the genetic susceptibility in people with heterochromatic variations, which in turn cause chromosome instability and predispose the individual to cancer. We report a case of bilateral retinoblastoma with complete absence of pericentromeric heterochromatin on one of the chromosomes number 9. A similar deficiency of pericentromeric heterochromatin on chromosome number 9 and 16 has been reported in a phenotypically normal individual and a Down syndrome case, respectively. This deficiency was found to be inherited from the father in all the three cases. Complete absence of pericentromeric heterochromatin of chromosome 9 is not being reported in association with cancer syndromes. Further studies are necessary to understand the role of this factor in normals and in those with cancer susceptibility, specially with retinoblastoma and the paternal origin of this deficiency.

Type
Research Article
Copyright
Copyright © The International Society for Twin Studies 1997

References

REFERENCES

1. Advaryu, SG, Dave, BJ, Trivedi, AH, Jani, KH, Vyas, RC (1987): Heteromorphism of C-band positive chromosomal regions in CML patients. Cancer Genet Cytogenet 27: 3337.Google Scholar
2. Atkin, NB, Brito-Babapulle, V (1981): Heterochromatin polymorphism and human cancer. Cancer Genet Cytogenet 3: 261272.Google Scholar
3. Buys, CHCM, Ypma, JMM, Gouw, WL (1979 a): Complete deficiency of constitutive heterochro-matin on a Human chromosome 9. Hum Genet 49: 129132.Google Scholar
4. Buys, CHCM, Anders, GJPA, Gouw, WL, Borkent-Ypma, JMM, Blenkers-Platter, JAM (1979b): A comparison of constitutive heterochromatin staining methods in two cases of familial hete-rochromatin deficiencies. Hum Genet 52: 133138.Google Scholar
5. Dave, BJ, Trivedi, AH, Advaryu, SG (1991): Variations in centromeric heterochromatin among patients with premalignant and malignant oral diseases. Int J Cancer 48: 386389.Google Scholar
6. Erdtmann, B (1982): Aspects of evaluation, significance and evolution of human C-band heteromorphism. Hum Genet 61: 281294.Google Scholar
7. Hsu, TC (1975): A possible function of constitutive heterochromatin: The bodyguard hypothesis. Genetics (Suppl.) 79: 137150.Google Scholar
8. Kopf, I, Islam, MQ, Friberg, LG, Levan, G (1989): Familial occurence of cancer and heteromor-phism of the heterochromatic segment of chromosome 1. Hereditas 110: 7983.Google Scholar
9. Luke, S, Verma, RS, Conte, RA, Mathews, T (1992): Molecular characterization of the secondary constriction region (qh) of human chromosome 9 with pericentric inversion. J Cell Sci 103: 919923.CrossRefGoogle ScholarPubMed
10. Magenis, RE, Palmer, CG, Wang, L, Brown, M, Chamberlin, J, Parks, M, Merritt, AD, Rivas, M, Yu, PL (1977): Heritability of chromosome banding variants. In Hook, EB, Porter, IH (eds.) “Population cytogenetic studies in humans”. New York, San Francisco, London, Academic Press, pp 179188.Google Scholar
11. Mao, WS, Lin, XH, Ma, QY, Chen, YZ, Zeng, LH, Dai, ZY (1989): Lymphocyte chromosome survey in 80 patients with retinoblastoma. Yen-Ko-Hsueh-Pao 5: 713.Google ScholarPubMed
12. Munier, F, Pescia, G, Jotterand-Bellomo, M, Balmer, A, Gailloud, C, Thonney, F (1989): Constitutional karyotype in retinoblastoma: case report and review of literature. Oph Ped Genet 10: 129149.Google Scholar
13. Shabtai, F, Halbrecht, I (1979): Risk of malignancy and chromosomal polymorphism: a possible mechanism of association. Clin Genet 15: 7377.Google Scholar
14. Shabtai, F, Antebi, E, Klar, D, Hart, J, Halbrecht, I (1985): Cytogenetic study in patients with carcinoma of colon and rectum: particular C-band variants as possible markers for cancer proneness. Cancer Genet Cytogenet 14: 235245.Google Scholar
15. Verma, N, Ghose, S, Sekhar, GC (1984): Ultrasonic evaluation of Retinoblastoma. Jap J Ophthal-mol 28: 222229.Google Scholar