Tinjauan Sosio Historis Strategi Pengembangan Kemampuan Menulis dalam Konteks Implementasi Kebijakan Penulisan Jurnal Pendidikan Tinggi

Surat Edaran Dikti 152/E/T/2012 telah disikapi pro dan kontra, seolah kebijakan Dikti merupakan tagihan pada sisi hilir namun melupakan fakta bahwa menulis bukan sekedar persoalan pada sisi hilir, namun merupakan persoalan hulu sampai dengan hilir yang melibatkan pengalaman, pendidikan dan latihan, dan motivasi sehingga memerlukan kajian secara komprehensif. Menulis merupakan proses mental yang dipengaruhi oleh faktor sosial historis yaitu pengalaman. Latihan, dan motivasi. Menulis bukanlah persoalan sederhana semudah membalikkan telapak tangan, namun menulis menyangkut persoalan kultural. Strategi pengembangan yang dilakukan seharusnya juga mencerminkan adanya aktualisasi ilmu pendidikan antara lain melalui; (1) pengembangan kemampuan menulis sejak dini secara tepat, (2) memberikan motivasi dengan menempatkan menulis sebagai pilihan karir prima, (3) pemerintah memberikan pelayanan primer terstandar seperti memberikan wadah terbitnya berbagai jurnal, (4) revitalisasi pengembangan minat baca, dan (5) menyediakan pendidikan dan latihan menulis yang memadai. Edaran Dikti 152/E/T/2012 harus dipandang sebagai langkah awal yang baik dan menjadi bagian koheren dari strategi pengembangan budaya menulis yang transformatif

Negative cell cycle regulation by Calcineurin is necessary for proper beta cell regeneration in zebrafish

peer reviewedStimulation of pancreatic beta cell regeneration could be a therapeutic lead to treat diabetes. Unlike humans, the zebrafish can efficiently regenerate beta cells, notably from ductal pancreatic progenitors. To gain insight into the molecular pathways involved in this process, we established the transcriptomic profile of the ductal cells after beta cell ablation in the adult zebrafish. These data highlighted the protein phosphatase calcineurin as a new potential modulator of beta cell regeneration. We showed that calcineurin overexpression abolished the regenerative response, leading to glycemia dysregulation. On the opposite, calcineurin inhibition increased ductal cell proliferation and subsequent beta cell regeneration. Interestingly, the enhanced proliferation of the progenitors was paradoxically coupled with their exhaustion. This suggests that the proliferating progenitors are next entering in differentiation. Calcineurin appears as a guardian which prevents an excessive progenitor proliferation to preserve the pool of progenitors. Altogether, our findings reveal calcineurin as a key player in the balance between proliferation and differentiation to enable a proper beta cell regeneration

Identification of downstream effectors of retinoic acid specifying the zebrafish pancreas by integrative genomics.

Retinoic acid (RA) is a key signal for the specification of the pancreas. Still, the gene regulatory cascade triggered by RA in the endoderm remains poorly characterized. In this study, we investigated this regulatory network in zebrafish by combining RNA-seq, RAR ChIP-seq and ATAC-seq assays. By analysing the effect of RA and of the RA receptor (RAR) inverse-agonist BMS493 on the transcriptome and on the chromatin accessibility of endodermal cells, we identified a large set of genes and regulatory regions regulated by RA signalling. RAR ChIP-seq further defined the direct RAR target genes in zebrafish, including hox genes as well as several pancreatic regulators like mnx1, insm1b, hnf1ba and gata6. Comparison of zebrafish and murine RAR ChIP-seq data highlighted the conserved direct target genes and revealed that some RAR sites are under strong evolutionary constraints. Among them, a novel highly conserved RAR-induced enhancer was identified downstream of the HoxB locus and driving expression in the nervous system and in the gut in a RA-dependent manner. Finally, ATAC-seq data unveiled the role of the RAR-direct targets Hnf1ba and Gata6 in opening chromatin at many regulatory loci upon RA treatment

Susceptibility and permissivity of zebrafish (Danio rerio) larvae to cypriniviruses

No abstract available

La intervención personal de Dios en la historia de israel. El «yo» de Yahvéh en el libro de Amós

1. EN LOS ORÁCULOS CONTRA ISRAEL Y LOS PUEBLOS VECINOS (AM 1-2). a) La decisión de Yahvéh de castigar a Israel y a los pueblos vecinos por sus rebeldías, es irrevocable. b) La destrucción por un fuego. c) Además del fuego,Yahvéh castigará también de otra manera a los culpables. d) Intervenciones de Yahvéh en el pasado a favor de Israel. 2. EN LAS AMONESTACIONES Y AMENAZAS A ISRAEL (AM 3-6). a) Las tradiciones constitutivas de Israel como pueblo. b) Las ocasiones no aprovechadas (Am 4, 6-12). c) La crítica del culto de Israel (Am 5, 21-27). d) El juramento de Yahvéh. e) Los anuncios del castigo inminente. 3. EN LAS VISIONES DE AMÓS (AM 7, 1 - 9, 1-10). a) En el texto mismo de las cinco visiones. b) En el otro material oracular de esta parte. 4. EN LOS ORÁCULOS DE RESTAURACIÓN (AM 9, 11-15). CONCLUSIÓN

Fast Homozygosity Mapping and Identification of a Zebrafish ENU-Induced Mutation by Whole-Genome Sequencing

Forward genetics using zebrafish is a powerful tool for studying vertebrate development through large-scale mutagenesis. Nonetheless, the identification of the molecular lesion is still laborious and involves time-consuming genetic mapping. Here, we show that high-throughput sequencing of the whole zebrafish genome can directly locate the interval carrying the causative mutation and at the same time pinpoint the molecular lesion. The feasibility of this approach was validated by sequencing the m1045 mutant line that displays a severe hypoplasia of the exocrine pancreas. We generated 13 Gb of sequence, equivalent to an eightfold genomic coverage, from a pool of 50 mutant embryos obtained from a map-cross between the AB mutant carrier and the WIK polymorphic strain. The chromosomal region carrying the causal mutation was localized based on its unique property to display high levels of homozygosity among sequence reads as it derives exclusively from the initial AB mutated allele. We developed an algorithm identifying such a region by calculating a homozygosity score along all chromosomes. This highlighted an 8-Mb window on chromosome 5 with a score close to 1 in the m1045 mutants. The sequence analysis of all genes within this interval revealed a nonsense mutation in the snapc4 gene. Knockdown experiments confirmed the assertion that snapc4 is the gene whose mutation leads to exocrine pancreas hypoplasia. In conclusion, this study constitutes a proof-of-concept that whole-genome sequencing is a fast and effective alternative to the classical positional cloning strategies in zebrafish

Expression of zebrafish pax6b in pancreas is regulated by two enhancers containing highly conserved cis-elements bound by PDX1, PBX and PREP factors

BACKGROUND: PAX6 is a transcription factor playing a crucial role in the development of the eye and in the differentiation of the pancreatic endocrine cells as well as of enteroendocrine cells. Studies on the mouse Pax6 gene have shown that sequences upstream from the P0 promoter are required for expression in the lens and the pancreas; but there remain discrepancies regarding the precise location of the pancreatic regulatory elements. RESULTS: Due to genome duplication in the evolution of ray-finned fishes, zebrafish has two pax6 genes, pax6a and pax6b. While both zebrafish pax6 genes are expressed in the developing eye and nervous system, only pax6b is expressed in the endocrine cells of the pancreas. To investigate the cause of this differential expression, we used a combination of in silico, in vivo and in vitro approaches. We show that the pax6b P0 promoter targets expression to endocrine pancreatic cells and also to enteroendocrine cells, retinal neurons and the telencephalon of transgenic zebrafish. Deletion analyses indicate that strong pancreatic expression of the pax6b gene relies on the combined action of two conserved regulatory enhancers, called regions A and C. By means of gel shift assays, we detected binding of the homeoproteins PDX1, PBX and PREP to several cis-elements of these regions. In constrast, regions A and C of the zebrafish pax6a gene are not active in the pancreas, this difference being attributable to sequence divergences within two cis-elements binding the pancreatic homeoprotein PDX1. CONCLUSION: Our data indicate a conserved role of enhancers A and C in the pancreatic expression of pax6b and emphasize the importance of the homeoproteins PBX and PREP cooperating with PDX1, in activating pax6b expression in endocrine pancreatic cells. This study also provides a striking example of how adaptative evolution of gene regulatory sequences upon gene duplication progressively leads to subfunctionalization of the paralogous gene pair