Analise molecular do loco C4/CYP21 : impacto da variabilidade alelica provocada por recombinações sobre os metodos de avaliação de mutações / Molecular analysis of C4/CYP21 locus : influence of allelic variability caused by recombinations on current methods of mutation detection

Coeli, Fernanda Borchers

13 August 2018

Orientador: Maricilda Palandi de Mello / Tese (doutorado) - Universidade Estadual de Campinas, Insituto de Campinas / Made available in DSpace on 2018-08-13T00:56:19Z (GMT). No. of bitstreams: 1 Coeli_FernandaBorchers_D.pdf: 7777269 bytes, checksum: 053a66d2bc3df6ad0d5de7c2038f3246 (MD5) Previous issue date: 2009 / Resumo: A hiperplasia congênita da adrenal é causada pela deficiência de uma das cinco enzimas responsáveis pela síntese do cortisol na esteroidogênese, sendo que mais de 90% dos casos ocorrem devido à deficiência de 21-hidroxilase (21-OH). O genoma haplóide humano possui duas cópias em tandem do gene que codifica para a 21-OH, denominados CYP21A2 e o CYP21A1P. Embora as duas cópias, CYP21A1P e CYP21A2, tenham aproximadamente 98% de homologia, CYP21A1P é classificado como um pseudogene, devido a algumas alterações deletérias em sua seqüência. Foram mapeados no braço curto do cromossomo 6, assim como os genes RP, C4 e TNX também duplicados em tandem. Este loco é denominado modulo RCCX, onde cada letra representa um gene. Uma conseqüência esperada deste tipo de organização é que esta favorece eventos de crossingover desigual, produzindo cromátides irmãs assimétricas e pares de gametas com um número variável de unidades completas. O crossover desigual não gera somente um tipo definido de deleção (alelos monomodulares), de duplicação (alelo trimodular) ou de conversão (alelo bimodular), mas pode, dependendo da sua exata localização, produzir um grande número de alelos diferentes, com significados funcionais variáveis. O objetivo deste trabalho foi investigar a variabilidade dos genes híbridos CYP21A21P/CYP21A2 quanto à região de recombinação nos alelos monomodulares, bimodulares e trimodulares de indivíduos com deficiência de 21- hidroxilase. Foram incluídos 55 pacientes com deficiência de 21 - hidroxilase, que foram avaliados por Southern blot, Multiplex ligation-dependent probe amplification (MLPA), PCR - Alelo especifico (ASO-PCR) e seqüenciamento. Na triagem por Southern blot foram identificados 26 alelos mono-, 26 bi- e 5 trimodulares com prováveis genes híbridos. Foi identificado um alelo monomodular novo portador da variante C4A [6,4 kb] que se mostrou único inclusive quanto à formação híbrida CYP21A21P/CYP21A2. Com a técnica de MLPA foi possível mapear três regiões principais de recombinação dos genes híbridos CYP21A21P/CYP21A2 nas três configurações alélicas. Além disso, foram identificados possíveis híbridos dos genes C4A e B, tanto nas configurações mono quanto nas bimodulares. Assim, ficaram definidos 5 haplótipos monomodulares, 7 bimodulares e 3 trimodulares. As técnicas de ASO-PCR e sequenciamento para análise dos híbridos CYP21A21P/CYP21A2 e dos CYP21A21P nos alelos bi e trimodulares refinaram a caracterização subdividindo estes haplótipos em 10 mono, 15 bi e 5 trimodulares. Dado o alto grau de variabilidade encontrado não foi possível se identificar efeito fundador de nenhum haplótipo específico para a deficiência de 21-hidroxilase. Por outro lado, um haplótipo novo correspondendo a cerca de 15% dos monomodulares foi caracterizado como portador das mutações p.P34L e p.H62L e um haplótipo igualmente não descrito portador da p.H62L foi encontrado entre os bimodulares. SNPs no terminal 5'UTR, no íntron 2 e no éxon 7 responderam pela diferenciação principal entre os híbridos tanto nos haplótipos de mesmo grupo como na comparação entre os de grupos diferentes. Este trabalho indica que a combinação de quatro técnicas e o estudo de segregação nas famílias foram fundamentais para o esclarecimento dos genótipos dos pacientes. Os genes híbridos podem estar relacionados às formas clínicas perdedora de sal, não perdedora de sal e não clássica dependendo da região onde ocorre a recombinação para sua formação. / Abstract: Congenital adrenal hyperplasia is caused by deficiency of one of the five enzymes responsible for cortisol synthesis in the steroidogenesis. More than 90% of the cases occur due to deficiency of 21-hidroxilase (21-OH). The haploid human genome bears two copies in tandem of 21-OH coding gene, CYP21A2 and CYP21A1P. Although the two copies are approximately 98% homologous, CYP21A1P is a pseudogene, due to some deleterious mutations. They map to the short arm of chromosome 6, as well as RP, C4 and TNX genes which are also duplicated in tandem. This locus is called RCCX module, each letter representing one gene. An expected consequence of such organization is that it favors events of unequal crossing-overs, producing pairs of gametes with different number of complete units. The aim of this investigation was to estimate the variability of CYP21A21P/CYP21A2 chimeric genes based on the region of recombination in the monomodular, bimodular and trimodular alleles in patients with 21-hydroxylase deficiency. Fifty-five patients were included for Southern blot, Multiplex ligationdependent probe amplification (MLPA), Allele-specific PCR (ASO-PCR) and sequencing analyses. Southern blot identified alleles which were: mono (n = 26), bi (n = 26) and trimodular (n = 5) with chimeric genes. A novel monomodular allele was identified that carry C4A [6,4 kb] variant and also bore an unique CYP21A21P/CYP21A2 formation. MLPA technique mapped three main recombination regions in CYP21A21P/CYP21A2 chimerical genes in the three RCCX configurations. Moreover, it indicated possible chimeric C4A and B genes in both mono- and bimodular configurations. Therefore, five mono-, seven bi- and three trimodular haplotypes had been defined. Both ASO-PCR and sequencing techniques for CYP21A21P/CYP21A2 and CYP21A21P analysis had refined the characterization subdividing these haplotypes in ten mono-, fifteen bi- and five trimodular. Considering the high degree of variability observed it was not possible to identify a founder effect of any specific haplotype for the deficiency of 21-hidroxilase. Conversely, a novel haplotype corresponding to about 15% of the monomodular alleles was characterized as carrying the mutations p.P34L and p.H62L and, similarly one haplotype carrying the p.H62L was found among bimodular alleles. SNPs in the 5 ' UTR, intron 2 and exon 7 were responsible for the main differentiation among chimerical genes within a group as well as upon comparison between different groups. The results presented here indicate that the combination of four different techniques and the study of segregation in the families had been essential for defining the genotypes of the patients. It is also shown that CYP21A21P/CYP21A2 chimeric genes can be related to different clinical forms: salt losing, non-salt losing and non-classical depending on the region where the recombination for its formation occurs. / Doutorado / Genetica Animal e Evolução / Doutor em Genetica e Biologia Molecular

Gene hibrido CYP21A1P/CYP21A2

Deficiencia de 21 hidroxilase

Modulo RCCX

Deleção de genes

Conversão genica

CYP21A1P/CYP21A2 chimeric gene

21-hydroxylase deficiency

RCCX module

Gene deletion

Gene conversion

Die Bedeutung partieller 21-Hydroxylase- und 3beta-Hydroxysteroiddehydrogenasedefizienzen für die Ätiopathogenese von Fertilitätsstörungen

Ghanaati, Zahra

12 March 2001

Ziel der Untersuchungen war, zur Klärung der Ursachen einer während der letzten Jahrzehnte erhöhten Frequenz sowohl von PCOS als auch von IO beizutragen. Es war zu ermitteln, ob hormonelle Verschiebungen bei den Patienten nachweisbar und diese durch genetische und epigenetische Faktoren erklärbar sind. Ausgehend von dem Postulat, daß verminderte 21-OH- und 3beta-HSD-Aktivitäten als prädisponierende Faktoren von PCOS und IO angesehen werden, waren hormonanalytische Untersuchungen zur Ermittlung partieller 21-OH- bzw. 3beta-HSD-Defizienzen durchgeführt worden. Den eigenen Erfahrungen und Darstellungen der internationalen Literatur entsprechend befaßt sich ein Teil der Methodik mit der Entwicklung einer neuen, der üblichen 17alfa-OHP-Messung überlegenen Methode zur Ermittlung von 21-OH-Defizienzen durch 21-DOF-Bestimmung nach ACTH-Test im Blutplasma. Wir erhielten bei vier von 21 PCOS-Patientinnen und drei von acht Patienten mit IO erhöhte 21-DOF-, 21-DOF/F- bzw. 17alfa-OHP-Werte nach ACTH-Test, die auf partielle 21-OH-Defizienzen hinweisen. Zusätzlich wurden bei 12 PCOS-Patientinnen erhöhte basale DHEAS- oder DHEAS/F-Werte gefunden, die als Hinweise auf partielle 3beta-HSD-Defizienzen oder 17,20-Lyase-Hyperaktivität gedeutet wurden. In der Stichprobe der IO waren DHEAS oder DHEAS/F-Werte bei vier Patienten erhöht. Da bei vier der 12 Patientinnen mit PCOS und zwei von vier Patienten mit IO genetisch und endokrinologisch gleichzeitig eine partielle 21-OH-Defizienz nachgewiesen wurde, kann bei diesen Patienten eine partielle 3beta-HSD-Defizienz weitgehend ausgeschlossen werden. Es wurden molekulargenetische Untersuchungen für die 14 häufigsten Mutationen in CYP21 bei Cohorten mit AGS, PCOS und IO durchgeführt. Die Untersuchung der AGS-Patienten sollte dazu dienen, ein effizientes und schnelles System der Mutationssuche für diagnostische Zwecke zu etablieren. Es wurden die häufigsten, phänotypisch wirksamen Mutationen in CYP21 bei der Mehrzahl dieser Patientengruppe im homozygoten bzw. compound heterozygoten Zustand gefunden und eine deutliche Genotyp-Phänotyp-Korrelation festgestellt. Auch bei Patientinnen mit PCOS sowie bei IO, bei denen partielle 21-OH-Defizienzen nachweisbar waren, wurden Mutationen in CYP21 gefunden. Die hierbei heterozygot vorliegenden Mutationen waren dieselben, die homozygot oder compound heterozygot bei schweren Formen des AGS gefunden wurden. Es ergab sich eine Korrelation molekulargenetischer und hormonanalytischer Befunde bei AGS, PCOS sowie IO. Allerdings konnten bei der Mehrzahl der Fälle mit PCOS und mit IO weder Mutationen noch hormonelle Auffälligkeiten hinsichtlich partieller 21-OH-Defizienzen gefunden werden. Die jedoch bei vielen Patientinnen gefundenen erhöhten DHEAS- und DHEAS/F-Werte stimmen mit Untersuchungen überein, die parallel starke Zunahmen der Häufigkeit der Hemmung des Enzyms 3ß-HSD bzw. der Aktivierung der 17,20-Lyase bei PCOS-Patientinnen und der Prävalenz des PCOS selbst bei nach 1955 geborenen Frauen und von Spermatogenesestörungen bei nach 1960 geborenen Männern fanden. Die Ursache hierfür wird in der Beeinflussung der adrenalen und gonadalen Steroidhormonsynthese vor allem durch das Umweltteratogen DDT und seine Metaboliten gesehen. Weiterhin wurde der Umweltfaktor Streß diskutiert. Für die Ätiopathogenese der untersuchten Fertilitätsstörungen werden materno-fetale Mechanismen postuliert, worauf unsere sowohl molekulargenetischen als auch hormonanalytischen Befunde hinweisen. Insgesamt bestätigen die Ergebnisse unserer Arbeit die These, daß Leben auf der Interaktion von Genen und Umweltfaktoren beruht und daß Hormone dabei als Mediatoren wirken. In gen- oder umweltbedingten unphysiologischen Konzentrationen können sie während kritischer Entwicklungsphasen des neuroendokrinen Systems als Teratogene wirken und zu lebenslangen Reproduktionsstörungen führen. / This paper describes a mutational and hormonal screening in a cohort of 21 patients ultrasonically diagnosed with PCO. Our data show single heterozygous base pair CYP21 mutations in 4 patients. The four women with PCOS and CYP21 mutations also displayed clear signs of partial 21-hydroxylase deficiency through a significant rise in 21DOF or 17alfa-OHP plasma levels after ACTH stimulation. Azziz et al. have reported several heterozygous mutations in hyperandrogenic women with LO-CAH. Other studies report several heterozygous point mutations in hyperandrogenic woman who, however, were not examined for polycystic ovaries.The correlation between the hormone profiles and genetic screening results found with our patients underscores the latter s usefulness with PCOS patients. In contrast to the hormone profile, genetic screening is not influenced by external factors. The frequency of heterozygous CYP21 mutations is higher (19%) than in the normal population (5-8%), suggesting a link with PCOS in some cases. The ratio of LH/FSH was significantly raised in 43% of the cases. Most importantly, basal plasma DHEA-S levels and DHEA-S/F ratios were clearly increased, higher than the means +2SD in controls. This suggests a partial 3beta-hydroxysteroid dehydrogenase deficiency or 17,20 lyase hyperactivity. Other authors, however, were not able to find mutations in the corresponding genes. This could be explained by the fact that the DDT metabolite o,p DDD is a strong inhibitor of 3beta-HSD, and that DDT and its metabolites may be able to activate the 17,20 lyase, a cytochrome P450 enzyme. Furthermore, DDT has some oestrogen activity, and its perinatal administration can produce a PCOS-like syndrome in rats. Very significantly, there has not only been an approximately fourfold increased prevalence of PCO in women borne since 1955 in eastern Germany, following a massive prenatal exposure to DDT, but also a notable shift in the hormone profiles of those affected. A predominance of 3beta-HSD deficiencies and 17,20 lyase hyperactivity (70%) vs. 21-hydroxylase deficiency (23%) has emerged, in contrast with 21-hydroxylase deficiencies in 70% vs. 3beta-HSD deficiencies or 17,20 lyase hyperactivity in 14% for those born earlier than 1955. Similar results were obtained in this study for women with PCOS born since 1955, suggesting that the prenatal exposure of high amounts of DDT and its metabolites indeed appear to be responsible - at least in part - for the major increase in PCO and PCOS.

heterozygous mutations

partial 21-hydroxylase deficiency

Polycystic Ovary Syndrome (PCOS)

heterozygous mutations

partial 21-hydroxylase deficiency

Polycystic Ovary Syndrome (PCOS)

570 Biowissenschaften, Biologie

32 Biologie

XG 8500

YC 4400

ddc:570