Founder effect for the highly prevalent R337H mutation of tumor suppressor p53 in Brazilian patients with adrenocortical tumors

Pinto, Emilia M.; Billerbeck, Ana Elisa C.; Villares, Maria Candida B.F.; Domenice, Sorahia; Mendonça, Berenice B.; Latronico, Ana Claudia

doi:10.1590/S0004-27302004000500009

Abstracts

The incidence of adrenocortical tumors in children from the Southern region of Brazil is higher than in other parts of the world. This fact has been related to the identification of an inherited missense mutation of the p53 (R337H) at high frequency (78-97%) in Brazilian children with adrenocortical tumors. Given the high frequency of this germline mutation in the Brazilian population, it is very likely that the R337H mutation has arisen from a common origin. In this study, we analyzed two highly polymorphic intragenic markers (VNTRp53 and p53CA) in 22 patients (16 children and 6 adults) with adrenocortical tumors carrying the germline R337H mutation and 60 normal individuals using GeneScan Fragment Analysis software. We found six and sixteen different alleles for the VNTRp53 and p53CA polymorphic markers, respectively. Two distinct alleles, both with 122 bp, were found in 56.8% (VNTRp53) and 54.5% (p53CA) of the 44 alleles from patients with adrenocortical tumors associated with the R337H mutation. Differently, these same VNTRp53 and p53CA alleles were found in 18.3% and 14.2% of 120 alleles from normal individuals, respectively (p<0.01, Chi-square test). An identical haplotype for p53 locus was also identified in 95% of the apparently unrelated Brazilian patients with adrenocortical tumors carrying the R337H mutation. In conclusion, we demonstrated a strong evidence of co-segregation between two intragenic polymorphic p53 markers and the germline R337H mutation, indicating that this mutation has originated from a single common ancestral in the great majority of the Brazilian patients with adrenocortical tumors.

Adrenal tumors; p53; Polymorphic markers; Founder effect

A incidência dos tumores adrenocorticais em crianças das regiões sul e sudeste do Brasil é maior que em outras partes do mundo. Este fato tem sido atribuído a identificação com alta frequência (78-97%) da mutação R337H no p53 em crianças brasileiras com tumores adrenocorticais. Considerando a elevada freqüência desta mutação germinativa na população brasileira, é provável que a mutação R337H tenha uma origem comum. Neste estudo, analisamos 2 marcadores polimórficos intragênicos (VNTRp53 e p53CA) em 22 pacientes (16 crianças e 6 adultos) com tumores adrenocorticais portadores da mutação germinativa R337H e em 60 indivíduos normais, através do programa GeneScan de análise de fragmentos. Seis e 16 alelos dos marcadores polimórficos VNTRp53 e p53CA foram respectivamente identificados. Dois alelos, ambos com 122 bp, foram identificados em 56,8% (VNTRp53) e 54,5% (p53CA) dos 44 alelos dos pacientes com tumores adrenocorticais. Em contraste, estes mesmos marcadores foram encontrados respectivamente em 18,3% e 14,2% dos 120 alelos dos indivíduos normais (p< 0,01, teste do chi-quadrado). Identificamos também, um haplótipo idêntico para o locus p53 em 95% dos pacientes com tumores adrenocorticais com a mutação R337H. Em conclusão, demonstramos uma forte evidência de co-segregação entre dois marcadores polimórficos intragênicos do p53 e a mutação germinativa R337H, indicando que esta mutação teve origem num ancestral comum na maioria dos pacientes brasileiros com tumores adrenocorticais.

Tumores adrenais; p53; Marcadores polimórficos; Efeito fundador

ARTIGO ORIGINAL

Founder effect for the highly prevalent R337H mutation of tumor suppressor p53 in Brazilian patients with adrenocortical tumors

Efeito fundador da altamente prevalente mutação R337H do gene supressor de tumores p53 em pacientes brasileiros com tumores adrenocorticais

Emilia M. Pinto; Ana Elisa C. Billerbeck; Maria Candida B.F. Villares; Sorahia Domenice; Berenice B. Mendonça; Ana Claudia Latronico

Unidade de Endocrinologia do Desenvolvimento, Laboratório de Hormônios e Genética Molecular LIM/42, Disciplina de Endocrinologia e Metabologia, Hospital das Clínicas, Faculdade de Medicina da Universidade de São Paulo, São Paulo, Brasil

^{Correspondence} Correspondence to Ana Claudia Latronico Laboratório de Hormônios e Genética Molecular LIM/42 - Hospital das Clínicas, Faculdade de Medicina - USP Av. Dr. Enéas Carvalho de Aguiar, 155, 2º andar, Bloco 6, 05403-900 São Paulo, SP - Brasil FAX: (5511) 3083-0626 E-mail: anacl@usp.br

ABSTRACT

The incidence of adrenocortical tumors in children from the Southern region of Brazil is higher than in other parts of the world. This fact has been related to the identification of an inherited missense mutation of the p53 (R337H) at high frequency (78-97%) in Brazilian children with adrenocortical tumors. Given the high frequency of this germline mutation in the Brazilian population, it is very likely that the R337H mutation has arisen from a common origin. In this study, we analyzed two highly polymorphic intragenic markers (VNTRp53 and p53CA) in 22 patients (16 children and 6 adults) with adrenocortical tumors carrying the germline R337H mutation and 60 normal individuals using GeneScan Fragment Analysis software. We found six and sixteen different alleles for the VNTRp53 and p53CA polymorphic markers, respectively. Two distinct alleles, both with 122 bp, were found in 56.8% (VNTRp53) and 54.5% (p53CA) of the 44 alleles from patients with adrenocortical tumors associated with the R337H mutation. Differently, these same VNTRp53 and p53CA alleles were found in 18.3% and 14.2% of 120 alleles from normal individuals, respectively (p<0.01, Chi-square test). An identical haplotype for p53 locus was also identified in 95% of the apparently unrelated Brazilian patients with adrenocortical tumors carrying the R337H mutation. In conclusion, we demonstrated a strong evidence of co-segregation between two intragenic polymorphic p53 markers and the germline R337H mutation, indicating that this mutation has originated from a single common ancestral in the great majority of the Brazilian patients with adrenocortical tumors.

Keywords: Adrenal tumors; p53; Polymorphic markers; Founder effect.

RESUMO

A incidência dos tumores adrenocorticais em crianças das regiões sul e sudeste do Brasil é maior que em outras partes do mundo. Este fato tem sido atribuído a identificação com alta frequência (78-97%) da mutação R337H no p53 em crianças brasileiras com tumores adrenocorticais. Considerando a elevada freqüência desta mutação germinativa na população brasileira, é provável que a mutação R337H tenha uma origem comum. Neste estudo, analisamos 2 marcadores polimórficos intragênicos (VNTRp53 e p53CA) em 22 pacientes (16 crianças e 6 adultos) com tumores adrenocorticais portadores da mutação germinativa R337H e em 60 indivíduos normais, através do programa GeneScan de análise de fragmentos. Seis e 16 alelos dos marcadores polimórficos VNTRp53 e p53CA foram respectivamente identificados. Dois alelos, ambos com 122 bp, foram identificados em 56,8% (VNTRp53) e 54,5% (p53CA) dos 44 alelos dos pacientes com tumores adrenocorticais. Em contraste, estes mesmos marcadores foram encontrados respectivamente em 18,3% e 14,2% dos 120 alelos dos indivíduos normais (p< 0,01, teste do chi-quadrado). Identificamos também, um haplótipo idêntico para o locus p53 em 95% dos pacientes com tumores adrenocorticais com a mutação R337H. Em conclusão, demonstramos uma forte evidência de co-segregação entre dois marcadores polimórficos intragênicos do p53 e a mutação germinativa R337H, indicando que esta mutação teve origem num ancestral comum na maioria dos pacientes brasileiros com tumores adrenocorticais.

Descritores: Tumores adrenais; p53; Marcadores polimórficos; Efeito fundador.

ADRENOCORTICAL TUMORS IN CHILDREN and adolescents are rare events. It is estimated that approximately 25 cases of pediatric adrenocortical tumors occur in the United States per year (1, 2). However, the high incidence of adrenocortical tumors in children from Southern region of Brazil is particularly remarkable, since it has been estimated to be approximately 10-15 times greater than the worldwide incidence (3). The identification of a unique p53 germline mutation, R337H, at a very high frequency (97-78%) of Brazilian children with adrenocortical tumors suggests that genetic predisposition plays an important role in the etiology of these tumors in the Brazilian population (4, 5).

Interestingly, the R337H mutation was also identified in the DNA of asymptomatic first degree relatives of patients with adrenocortical tumors and R337H, suggesting low penetrance of this p53 mutation for adrenocortical tumor development (4, 5). Adrenocortical tumors of patients with R337H mutation frequently display deletion of the entire chromosome 17 (3). In addition, in vitro analysis revealed that the p53 tetramerization domain containing the R337H mutation was less stable than the wild type domain (6). The stability of this mutant was highly sensitive to pH in the physiological range, suggesting that this missense mutation caused a pH-dependent p53 dysfunction (6).

Given the high frequency of the inherited R337H mutation in the Brazilians with adrenocortical tumors, it is most likely that this p53 mutation has originated from a single founder. To address this hypothesis, we compared the allelic distribution of two highly informative polymorphic markers into the p53 gene between apparently unrelated Brazilian patients with adrenocortical tumors carrying the R337H mutation and normal individuals in an attempt to clarify the origin of the p53 mutation

Patients and Methods

The study was approved by the Ethics Committee of Hospital das Clínicas, São Paulo, Brazil, and informed written consent was obtained from all patients. We selected 22 patients (16 children and 6 adults) who had adrenocortical tumors associated with the germiline R337H mutation. The median age was 1.2 years, ranging from 0.6 to 54 years. All patients were Caucasians. Sixty normal unrelated Brazilian individuals (30 children and 30 adults) were studied as controls.

DNA Analysis

Genomic DNA was extracted from peripheral blood leukocytes of all patients and controls according to standard protocols. Two highly informative polymorphic markers, VNTRp53 and p53CA, were amplified by polymerase chain reaction. The VNTRp53 is a pentanucleotide repeat (AAAAT)_n within intron 1 (7), whereas P53(CA)n is a dinucleotide repeat polymorphism of the human p53 gene (8). The oligonucleotide primers were labeled with fluorescent dye (TET or FAM). Genomic DNA was amplified in a 50 ml reaction mixture of 1x PCR buffer, 1.5 mM MgCl₂, 200 mM of each dNTP, 25-10 pmol of each primer and 0.5-0.8U Taq Polymerase (Amershan Pharmacia). The VNTRp53 PCR reaction mixture was denatured for 5 min at 93ºC, and cycled 35 times (93ºC for 1 min, 62ºC for 1 min and 72ºC for 1 min), followed by a 30 min extension at 72ºC. The p53CA PCR reaction mixture was denatured for 3 min at 94ºC, and cycled 35 times (94ºC for 1 min, 60ºC for 2 min and 72ºC for 5 min), followed by a 30 min extension at 72ºC. Internal size standard TAMRA 350 (Applied Biosystems, Foster City, CA) was added to 2 mL of PCR products and 24 mL of formamide and those were submitted to capillary electrophoresis in an Automatic Sequencer (ABI Prism 310 Genetic Analyzer) followed by GeneScan Fragment Analysis (Applied Biosystem, Foster City, CA).

Statistical Analysis

Differences in genotype frequencies between patients with adrenocortical tumors carrying the germline R337H mutation and normal controls for each polymorphic site were tested with Chi-square statistics.

Results

Six different alleles were identified for the VNTRp53 marker within the first intron of the p53 gene, ranging from 112 to 137 bp (Table 1). The alleles from 117 to 137 bp were previously described (7), whereas the allele corresponding to 112 bp has not been previously identified in other populations. The 122 bp allele containing 7 unit repeats was identified in 25 of the 44 alleles (56.8%) from patients with adrenocortical tumors associated with the germline R337H mutation. Differently, this same allele was found in 22 of 120 alleles (18.3%) from the normal controls.

Thumbnail

Sixteen different alleles were identified for the p53CA polymorphic marker, ranging from 102 to 134 bp (Table 1). The 122 bp allele was found in 24 of the 44 alleles (54.5%) from patients with adrenocortical tumors associated with the R337H mutation. Differently, this same allele was found in 17 of 120 alleles (14.2%) from the normal controls. The allele distribution was significantly different (p<0.01, Chi-square test) between patients with adrenocortical tumors and R337H mutation and normal controls. Segregation studies showed that an identical haplotype for the p53 locus was identified in 95% of the apparently unrelated Brazilian patients with adrenocortical tumors carrying the R337H mutation. In addition, this same haplotype was always present in tumor DNA, usually affected by LOH.

Discussion

We demonstrated a strong evidence of co-segregation between two distinct alleles within the p53 gene and the germline R337H mutation in Brazilian patients with adrenocortical tumors. The allelic frequencies were significantly different between these patients who harbored the R337H mutation and normal individuals, suggesting that the R337H mutation originated from a common ancestral in the Brazilian population.

The clear evidence of a founder effect for the R337H mutation contrasts with a previous study performed by Ribeiro et al. (4), who analyzed four different polymorphic markers along the short arm of chromosome 17, including the same two intragenic p53 markers studied here and two other flanking markers (D17S1832 and D17S786) in 17 patients carrying the R337H mutation. They demonstrated that at least some mutant alleles arose independently, thus eliminating the presence of a founder effect (4). However, the small number of unrelated patients studied, the physical distance of the two flanking markers in relation to p53 locus (8-12 centirays) and the absence of a control group, did not rule out the presence of a founder effect in this study. Additionally, an identical allele (represented by number 3) for the intragenic marker VNTRp53 was identified in 16 of 17 patients studied (4). However, these data were not accounted for in this study.

The majority of the population in the southern region of Brazil consists mainly of European extraction, such as Portuguese, Italian, Spanish and German, with native Brazilian Indian and African influence (9). The high incidence of adrenocortical tumors in patients from this region is therefore explained by the presence of the germline R337H mutation, which was inherited from a common founder several decades ago. This fact is suggested by identification of the R337H mutation in asymptomatic relatives of patients with adrenocortical tumors as old as 60 years old. Nevertheless, R337H has never been described as a common mutation of the p53 in other populations.

We have previously demonstrated that the second event, crucial for adrenocortical tumor development, is characterized by the loss of chromosome 17 harboring the normal p53 allele in most of affected patients (3). However, the etiologic factor for the occurrence of this second event, especially during childhood, remains unknown. Interestingly, the peak age of occurrence of adrenocortical tumors in Brazilian children is under of 4 years of age, suggesting that the second event also occurs very early in life or even during fetal life. Alterations of the pH in adrenocortical tissue, such as those observed during adrenal fetal apoptosis, have been speculated as participating in this still unknown process (6).

In conclusion, an identical haplotype for p53 locus was identified in 95% of the apparently unrelated Brazilian patients with adrenocortical tumors carrying the R337H mutation. The allelic frequencies were significantly different between affected patients carrying the R337H mutation and the normal population, indicating that this mutation originated from a single common ancestral in most of the Brazilian patients with adrenocortical tumors.

Recebido em 15/09/04

Aceito em 20/09/04

1. Young JL Jr, Miller RW. Incidence of malignant tumors in U.S. children. J Pediatr 1975;86:254-8
2. Lack EE, Mulvihill JJ, Travis WD, Kozakewich HP. Adrenal cortical neoplasms in the pediatric and adolescent age group. Clinicopathologic study of 30 cases with emphasis on epidemiological and prognostic factors. Pathol Annu 1992;27 Pt 1:1-53
3. Pinto EM, Billerbeck AEC, Fragoso MCBV, Mendonca BB, Latronico AC. Deletion-mapping of chromosome 17 in benign and malignant adrenocortical tumors associated with the Arg337His mutation of the p53 tumor suppressor protein. Endocrine Society Meeting. 2003: (Abs. P2-457)
4. Ribeiro RC, Sandrini F, Figueiredo B, Zambetti GP, Michalkiewicz E, Lafferty AR, DeLacerda L, Rabin M, Cadwell C, Sampaio G, Cat I, Stratakis CA, Sandrini R. An inherited p53 mutation that contributes in a tissue-specific manner to pediatric adrenal cortical carcinoma. Proc Natl Acad Sci USA 2001;98:9330-5.
5. Latronico AC, Pinto EM, Domenice S, Fragoso MC, Martin RM, Zerbini MC, Lucon AM, Mendonca BB. An inherited mutation outside the highly conserved DNA-binding domain of the p53 tumor suppressor protein in children and adults with sporadic adrenocortical tumors. J Clin Endocrinol Metab 2001;86:4970-3.
6. DiGiammarino EL, Lee AS, Cadwell C, Zhang W, Bothner B, Ribeiro RC, Zambetti G, Kriwacki RW. A novel mechanism of tumorigenesis involving pH-dependent destabilization of a mutant p53 tetramer. Nat Struct Mol Biol 2002;9:12-16
7. Hahn M, Fislage R, Pingoud A. Polymorphism of the pentanucleotide repeat d(AAAAT) within intron 1 of the human tumor suppressor gene p53 (17p13.1). Hum Genet 1995:471-472.
8. Jones MH, Nakamura Y. Detection of loss of heterozygosity at the human TP53 locus using a dinucleotide repeat polymorphism. Genes, Chromosomes & Cancer 1992;5:89-90
9. Parra FC, Amado RC, Lambertucci JR, Rocha J, Antunes CM, Pena SD. Color and genomic ancestry in Brazilians. Proc Natl Acad Sci USA 2003;100:177-82

Correspondence to

Ana Claudia Latronico

Laboratório de Hormônios e Genética Molecular

LIM/42 - Hospital das Clínicas, Faculdade de Medicina - USP

Av. Dr. Enéas Carvalho de Aguiar, 155, 2º andar, Bloco 6,

05403-900 São Paulo, SP - Brasil

FAX: (5511) 3083-0626

E-mail:

anacl@usp.br

Publication Dates

Publication in this collection
07 Mar 2005
Date of issue
Oct 2004

History

Accepted
20 Sept 2004
Received
15 Sept 2004

This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License.

[1] 1. Young JL Jr, Miller RW. Incidence of malignant tumors in U.S. children. J Pediatr 1975;86:254-8

[2] 2. Lack EE, Mulvihill JJ, Travis WD, Kozakewich HP. Adrenal cortical neoplasms in the pediatric and adolescent age group. Clinicopathologic study of 30 cases with emphasis on epidemiological and prognostic factors. Pathol Annu 1992;27 Pt 1:1-53

[3] 3. Pinto EM, Billerbeck AEC, Fragoso MCBV, Mendonca BB, Latronico AC. Deletion-mapping of chromosome 17 in benign and malignant adrenocortical tumors associated with the Arg337His mutation of the p53 tumor suppressor protein. Endocrine Society Meeting. 2003: (Abs. P2-457)

[4] 4. Ribeiro RC, Sandrini F, Figueiredo B, Zambetti GP, Michalkiewicz E, Lafferty AR, DeLacerda L, Rabin M, Cadwell C, Sampaio G, Cat I, Stratakis CA, Sandrini R. An inherited p53 mutation that contributes in a tissue-specific manner to pediatric adrenal cortical carcinoma. Proc Natl Acad Sci USA 2001;98:9330-5.

[5] 5. Latronico AC, Pinto EM, Domenice S, Fragoso MC, Martin RM, Zerbini MC, Lucon AM, Mendonca BB. An inherited mutation outside the highly conserved DNA-binding domain of the p53 tumor suppressor protein in children and adults with sporadic adrenocortical tumors. J Clin Endocrinol Metab 2001;86:4970-3.

[6] 6. DiGiammarino EL, Lee AS, Cadwell C, Zhang W, Bothner B, Ribeiro RC, Zambetti G, Kriwacki RW. A novel mechanism of tumorigenesis involving pH-dependent destabilization of a mutant p53 tetramer. Nat Struct Mol Biol 2002;9:12-16

[7] 7. Hahn M, Fislage R, Pingoud A. Polymorphism of the pentanucleotide repeat d(AAAAT) within intron 1 of the human tumor suppressor gene p53 (17p13.1). Hum Genet 1995:471-472.

[8] 8. Jones MH, Nakamura Y. Detection of loss of heterozygosity at the human TP53 locus using a dinucleotide repeat polymorphism. Genes, Chromosomes & Cancer 1992;5:89-90

[9] 9. Parra FC, Amado RC, Lambertucci JR, Rocha J, Antunes CM, Pena SD. Color and genomic ancestry in Brazilians. Proc Natl Acad Sci USA 2003;100:177-82