MicroRNA-196a regulates bovine newborn ovary homeobox gene (NOBOX) expression during early embryogenesis

Tripurani, Swamy K.; Lee, Kyung Bon; Wee, Gabbine; Smith, George W.; Yao, Jianbo

doi:10.1186/1471-213x-11-25

Cited by 75 publications

(60 citation statements)

References 54 publications

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“…Dysfunction and/or decrease in miRNAs of the miR-30 family could lead to podocyte apoptosis and depletion, glomerulosclerosis, and proteinuric renal disease. In other work, we found that the miR-30 family is expressed in renal tubular cells (J. Wu unpublished observations), and miR-196a was also shown to be expressed predominantly in the kidney (38). miR-196a was previously shown to correlate negatively with disease activity in SLE and has critical roles in cancer pathogenesis, viral immunity, and cell differentiation (39) as well as a role in kidney development.…”

Section: Discussionmentioning

confidence: 75%

Evaluation of MicroRNAs miR-196a, miR-30a-5P, and miR-490 as Biomarkers of Disease Activity among Patients with FSGS

Zhang

Chen

et al. 2014

Clinical Journal of the American Society of Nephrology

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Background and objectives This study aimed to identify urinary microRNAs (miRNAs) as biomarkers for FSGS disease activity.Design, setting, participants, & measurements Candidate urinary miRNAs were identified in pooled urine samples from patients with active FSGS (FSGS-A) and FSGS in remission (FSGS-CR), and were then validated using individual samples. Their levels were compared both under different treatment responses in a prospective study of FSGS and in patients with different membranous nephropathy (MN) and diabetic nephropathy (DN) disease activity. The prediction of these miRNAs for treatment responses was further analyzed in both retrospective and prospective cohorts of patients with FSGS.Results All 54 miRNAs were included as candidate biomarkers, including those with high levels in patients with FSGS-A (n=9) under the TaqMan Low Density Array as well as those with conserved expression in kidneys and involved in immune response. TaqMan probe-based quantitative RT-PCR confirmed the higher levels of four miRNAs in patients with FSGS-A in two independent cohorts (n=18 and n=80). Urinary miR-196a, miR-30a-5p, and miR-490 discriminated FSGS-A from FSGS-CR, with an area under the curve of $0.80. After steroid treatment, their levels were lower in steroid-responsive patients with FSGS (all P,0.001), but were unchanged in steroid-resistant patients. The levels of miRNAs were similar between active MN and MN in remission as well as active DN and incipient DN (all P.0.05). Urinary miR-30a-5p marginally predicted the response to steroid treatment in patients with FSGS-A, with an area under the curve of 0.63 (P=0.03). ConclusionsThe levels of urinary miR-196a, miR-30a-5p, and miR-490 are associated with FSGS disease activity.

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Section: Discussionmentioning

confidence: 75%

Evaluation of MicroRNAs miR-196a, miR-30a-5P, and miR-490 as Biomarkers of Disease Activity among Patients with FSGS

Zhang

Chen

et al. 2014

Clinical Journal of the American Society of Nephrology

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“…The action of miRNAs on maternal mRNA degradation has been clear in Zebrafish embryos, which shows that the miR430 is abundant in the embryonic activation point, just at the moment the degradation of the maternal transcripts takes place (44) . Recent studies have shown that in the bovine, maternal mRNA as NOBOX and NPM2 are regulated under the action of the miR-181st and miR196a, respectively (104,105) . It is important to point out that the route of the degradation mediated by miRNAs is present only during the activation of the embryonic genome, and is absent during the oogenesis and in the initial stages of the embryo (47,52,54,106) .…”

Section: Maternal Effect On the Activation Of The Embryonic Genomementioning

confidence: 99%

“…La acción de miRNAs sobre la degradación de RNAm maternos ha quedado clara en embriones del Zebrafish, donde se observa que el miR430 es abundante en el punto de la activación embrionaria, justo en el momento en que sucede la degradación de los transcritos maternos (44) . Estudios recientes han demostrado que en el bovino, RNAm maternos como NOBOX y NPM2 son regulados bajo la acción de los miR-181a y miR196a, respectivamente (104,105) . Es importante señalar que la vía de degradación mediada por los of mice brg1-/-are arrested at the 2-4 cells stage (108) .…”

Section: Efecto Materno Sobre La Activación Del Genoma Embrionariounclassified

“…Recently it was found that the messenger of the maternal gene NOBOX has binding sites for the miR-196a in his extreme UTR 3', demonstrating that this miRNA is a negative regulator during early embryogenesis in cattle. The miR-196a is present in the oocyte and embryo, its expression is increased in the embryonic stage of 4 to 8 cells (105) . The nucleoplasmin 2 (NPM2) is a specific protein from the egg that acts on the nuclear organization in early embryonic development (80) .…”

Section: Rnam Maternos En El Bovinomentioning

confidence: 99%

“…Recientemente se encontró que el mensajero del gen materno NOBOX tiene sitios de unión para el miR-196a en su extremo UTR 3', demostrando que este miRNA es un regulador negativo durante la embriogénesis temprana en el bovino. El miR-196a está presente en el ovocito y en el embrión, su expresión se incrementa en el estadio embrionario de 4 y 8 células (105) . La Nucleoplasmina 2 (NPM2) es una proteína específica del ovocito que actúa en la organización nuclear en el desarrollo embrionario temprano (80) .…”

Section: Rnam Maternos En El Bovinounclassified

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Efectos de los RNAm maternos sobre la maduración del ovocito y el desarrollo embrionario temprano en mamíferos

Burrola-Barraza¹,

González-Rodríguez

2015

Rev. Mex. Cienc. Pecu.

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Efectos de los RNAm maternos sobre la maduración del ovocito y el desarrollo embrionario temprano en mamíferos. RevisiónEffects of the maternal mRNA on the maturation of the oocyte and early embryonic development in mammals. Review M. Eduviges Burrola-Barraza a , Everardo González-Rodríguez a RESUMENObtener ovocitos madurados in vitro, que sean competentes para fertilizarse y originar un porcentaje superior al 50 % de blastocitos viables, es una de las principales metas que existen en el desarrollo in vitro de embriones bovinos. Es por ello necesario entender los procesos celulares, que desembocan en la maduración del ovocito durante la foliculogénesis y su subsecuente transición al embrión. La transición del ovocito al embrión es un proceso complejo que involucra la inactivación genómica del ovocito y la activación del genoma embrionario. Este proceso se da en bovinos en la etapa de 8 a 16 células y presenta una degradación selectiva de RNAm maternos, que fueron almacenados durante la ovogénesis y son la fuente para la codificación de proteínas en las etapas iníciales del desarrollo embrionario. La acción de los RNAm maternos es clave para que la activación del genoma embrionario se realice en tiempo y forma adecuados. Entender la participación de estos transcritos en la activación del genoma embrionario, es esencial para esclarecer los procesos celulares que fallan en los protocolos de maduración de ovocitos in vitro. Es por esto que el objetivo de esta revisión fue recopilar la información de los principales RNAm maternos que han sido identificados tanto en el modelo murino como el bovino, esto con el fin de integrar el conocimiento relacionado con los procesos genómicos que permiten el desarrollo del embrión en el bovino, y diseñar nuevas estrategias que permitan mejorar los protocolos de fertilización in vitro.PALABRAS CLAVE: Ovocito, Activación genoma embrionario, Bovino. ABSTRACTGet in vitro matured oocytes that could be competent for in vitro fertilization with a result of 50 % viable blastocysts, is one of the main problems in the in vitro development of bovine embryos. For these reason, is necessary to understand the cellular processes that lead to the maturation of the oocyte during folliculogenesis and subsequent transition to the embryo. The transition from oocyte to embryo is a complex process that involves genomic inactivation of the oocyte and embryonic genome activation. This process occurs in cattle in the stage of 8 to 16 cells where there are a selective degradation of maternal mRNA, which were stored during oogenesis and are the source of protein in the early stages of embryonic development. The action of maternal mRNA is a key for that embryonic genome activation takes place in form and time. Understanding the involvement of these transcripts in embryonic genome activation is essential to elucidate the cellular processes falling in oocyte maturation in vitro protocols. The aim of this review was to gather information from maternal genes that have been isolated both in the murine model and c...

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PCK1 is negatively regulated by bta-miR-26a, and a single-nucleotide polymorphism in the 3′ untranslated region is involved in semen quality and longevity of Holstein bulls

et al. 2016

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Phosphoenolpyruvate carboxykinase 1 (PCK1) is a multi-functional enzyme that plays important roles in physiological processes, including reproduction. We previously reported that the PCK1 transcript has five splice variants; PCK1-AS4, which lacks exon 5, is enriched in the testis of Holstein bulls. In the present study, we profiled select PCK1 transcript variants in the testis, epididymus, and semen of high- and low-performance bulls, and examined the possibility that microRNAs may be involved in single nucleotide polymorphism (SNP)-mediated modulation of PCK1 expression. PCK1-AS4 abundance is not significantly different between high- and low-performance bulls. Luciferase reporter assays, however, showed that bovine PCK1 expression is repressed by bta-miR-26a in HepG2 hepatocyte cells. One SNP (c. + 2183 G > T) at the miRNA-binding site of PCK1 does not influence PCK1 expression, but is associated with elevated ejaculation volume, fresh sperm motility, and genomic estimated breeding value of longevity, as well as with reduced values of composite index and calving ease. Collectively, the identified 3'-untranslated-region SNP variant highlights the importance of PCK1 in the fecundity of Holstein bulls, and implicates a role for bta-miR-26a in regulating PCK1 abundance. Further study is needed to assess the effects of other genetic variants in 5'-flanking region and exons of PCK1 on enzyme levels in the testis and sperm. Mol. Reprod. Dev. 83: 217-225, 2016. © 2016 Wiley Periodicals, Inc.

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MicroRNA-196a regulates bovine newborn ovary homeobox gene (NOBOX) expression during early embryogenesis

Cited by 75 publications

References 54 publications

Evaluation of MicroRNAs miR-196a, miR-30a-5P, and miR-490 as Biomarkers of Disease Activity among Patients with FSGS

Evaluation of MicroRNAs miR-196a, miR-30a-5P, and miR-490 as Biomarkers of Disease Activity among Patients with FSGS

Efectos de los RNAm maternos sobre la maduración del ovocito y el desarrollo embrionario temprano en mamíferos

PCK1 is negatively regulated by bta-miR-26a, and a single-nucleotide polymorphism in the 3′ untranslated region is involved in semen quality and longevity of Holstein bulls

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