Random X Inactivation and Extensive Mosaicism in Human Placenta Revealed by Analysis of Allele-Specific Gene Expression along the X Chromosome

Imprinted inactivation of the paternal X chromosome in marsupials is the primordial mechanism of dosage compensation for X-linked genes between females and males in Therians. In Eutherian mammals, X chromosome inactivation (XCI) evolved into a random process in cells from the embryo proper, where either the maternal or paternal X can be inactivated. However, species like mouse and bovine maintained imprinted XCI exclusively in extraembryonic tissues. The existence of imprinted XCI in humans remains controversial, with studies based on the analyses of only one or two X-linked genes in different extraembryonic tissues. Here we readdress this issue in human term placenta by performing a robust analysis of allele-specific expression of 22 X-linked genes, including XIST, using 27 SNPs in transcribed regions. We show that XCI is random in human placenta, and that this organ is arranged in relatively large patches of cells with either maternal or paternal inactive X. In addition, this analysis indicated heterogeneous maintenance of gene silencing along the inactive X, which combined with the extensive mosaicism found in placenta, can explain the lack of agreement among previous studies. Our results illustrate the differences of XCI mechanism between humans and mice, and highlight the importance of addressing the issue of imprinted XCI in other species in order to understand the evolution of dosage compensation in placental mammals

Stability of epigenetic control in normal and transformed human cells

A epigenética aborda o controle da expressão gênica através de diversos fatores que agem sob a cromatina, os melhor estudados são a metilação do DNA e a acetilação em histonas, relacionadas à repressão e ativação gênica, respectivamente. Em mamíferos, existem dois fenômenos epigenéticos interessantes: a inativação do cromossomo X (ICX) em fêmeas, que garante o equilíbrio transcricional gênico entre os sexos, e o imprinting genômico, caracterizado pela expressão monoalélica dependente da origem parental. No presente estudo, propusemos verificar a manutenção do controle epigenético em células humanas normais e transformadas em condições semelhantes de hipometilação do DNA e hiperacetilação em histonas (após uso das drogas 5-aza-2-\'deoxicitidina (5-aza-dC) e ácido valproico, respectivamente), através do monitoramento da expressão alelo-específica pelo uso de polimorfismos de única base presentes em regiões codificadoras. Em células normais houve manutenção da ICX e do imprinting genômico, enquanto que em células transformadas hipometiladas foram observadas indução de XIST, e perda de imprinting dos genes IGF2, H19 e PEG10. Observamos que ambas as drogas podem diminuir a expressão de DNMT1, e 5-aza-dC altera o equilíbrio entre acetilação e desacetilação da histona H4. Ainda, a ordem de adição dos reagentes ocasionou diferenças no nível de acetilação da histona H4 e na expressão gênica de XIST e PEG10. Nossos dados sugerem que: células humanas normais apresentam maior estabilidade do controle epigenético comparadas às células humanas transformadas, genes submetidos à ICX e \"imprintados\" não apresentam diferenças na rigidez do controle de expressão, e a cascata de reação seguida após perturbação de marcas epigenéticas pode ser alterada dependendo da modificação inicial.Epigenetics refers to mechanisms related to gene activity through conformational modifications in DNA without changes in the nucleotide sequence. Key players in the epigenetic control are DNA methylation and histone acetylation, which are related to gene activation and repression, respectively. Two striking epigenetic phenomena in mammalians are X chromosome inactivation (XCI) and genomic imprinting. XCI triggers the transcriptional silencing of all but one X chromosome in each female cell, while genomic imprinting is a process that leads to mono-allelic gene expression based on parental origin. In the present study, we intended to verify the maintenance of epigenetic control in normal and transformed human cells under the same conditions of epigenetic disturbance. For this purpose, 5-aza-2\'-deoxycytidine (5-aza-dC) and valproic acid (VPA) were used to cause DNA hypomethylation and histone hyperacetylation, respectively. By monitoring allelic-specific expression using single nucleotide polymorphisms present in coding regions, we were able to check the effects of the modifications in the expression pattern of imprinted or subjected to XCI genes. While in female normal cells XCI and genomic imprinting were not affected by VPA or 5-aza-dC treatments, transformed male cells showed XIST activation and loss of imprinting of PEG10, IGF2 and H19 genes in the hypomethylation scenario. In addition, both drugs can decrease the expression of DNMT1, and 5-aza-dC alters the balance between acetylation and deacethylation of histone H4. Furthermore, we could see different degrees of histone H4 acetylation levels and of XIST and PEG10 expression, depending on which of the drugs was added first. Our data suggest that the epigenetic control in normal human cells is more stable when compared to transformed human cells. In addition, both XCI and genomic imprinting are epigenetic features equally hard to disturb. Finally, depending on the initial epigenetic modification (global demethylation or acethylation), it will induce different epigenetic control networks, with consequence to the final status of gene expression

Genome-wide DNA methylation profile of leukocytes from melanoma patients with and without CDKN2A mutations

Melanoma is a highly aggressive cancer, accounting for up to 75% of skin cancer deaths. A small proportion of melanoma cases can be ascribed to the presence of highly penetrant germline mutations, and approximately 40% of hereditary melanoma cases are caused by CDKN2A mutations. The current study sought to investigate whether the presence of germline CDKN2A mutations or the occurrence of cutaneous melanoma would result in constitutive genome-wide DNA methylation changes. The leukocyte methylomes of two groups of melanoma patients (those with germline CDKN2A mutations and those without CDKN2A mutations) were analyzed together with the profile of a control group of individuals. A pattern of DNA hypomethylation was detected in the CDKN2A-negative patients relative to both CDKN2A-mutated patients and controls. Additionally, we delineated a panel of 90 CpG sites that were differentially methylated in CDKN2A-mutated patients relative to controls. Although we identified a possible constitutive epigenetic signature in CDKN2A-mutated patients, the occurrence of reported SNPs at the detected CpG sites complicated the data interpretation. Thus, further studies are required to elucidate the impact of these findings on melanoma predisposition and their possible effect on the penetrance of CDKN2A mutations

Seminário de Dissertação (2024)

Página da disciplina de Seminário de Dissertação (MPPP, UFPE, 2022) Lista de participantes == https://docs.google.com/spreadsheets/d/1mrULe1y04yPxHUBaF50jhaM1OY8QYJ3zva4N4yvm198/edit#gid=

NEOTROPICAL CARNIVORES: a data set on carnivore distribution in the Neotropics

Mammalian carnivores are considered a key group in maintaining ecological health and can indicate potential ecological integrity in landscapes where they occur. Carnivores also hold high conservation value and their habitat requirements can guide management and conservation plans. The order Carnivora has 84 species from 8 families in the Neotropical region: Canidae; Felidae; Mephitidae; Mustelidae; Otariidae; Phocidae; Procyonidae; and Ursidae. Herein, we include published and unpublished data on native terrestrial Neotropical carnivores (Canidae; Felidae; Mephitidae; Mustelidae; Procyonidae; and Ursidae). NEOTROPICAL CARNIVORES is a publicly available data set that includes 99,605 data entries from 35,511 unique georeferenced coordinates. Detection/non-detection and quantitative data were obtained from 1818 to 2018 by researchers, governmental agencies, non-governmental organizations, and private consultants. Data were collected using several methods including camera trapping, museum collections, roadkill, line transect, and opportunistic records. Literature (peer-reviewed and grey literature) from Portuguese, Spanish and English were incorporated in this compilation. Most of the data set consists of detection data entries (n = 79,343; 79.7%) but also includes non-detection data (n = 20,262; 20.3%). Of those, 43.3% also include count data (n = 43,151). The information available in NEOTROPICAL CARNIVORES will contribute to macroecological, ecological, and conservation questions in multiple spatio-temporal perspectives. As carnivores play key roles in trophic interactions, a better understanding of their distribution and habitat requirements are essential to establish conservation management plans and safeguard the future ecological health of Neotropical ecosystems. Our data paper, combined with other large-scale data sets, has great potential to clarify species distribution and related ecological processes within the Neotropics. There are no copyright restrictions and no restriction for using data from this data paper, as long as the data paper is cited as the source of the information used. We also request that users inform us of how they intend to use the data