Publications by authors named "Ian A Nicastro"

Organismal aging is marked by decline in cellular function and anatomy, ultimately resulting in death. To inform our understanding of the mechanisms underlying this degeneration, we performed standard RNA sequencing (RNA-seq) and Oxford Nanopore Technologies direct RNA-seq over an adult time course in Caenorhabditis elegans. Long reads allowed for identification of hundreds of novel isoforms and age-associated differential isoform accumulation, resulting from alternative splicing and terminal exon choice.

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Article Synopsis
  • Organismal aging leads to a decline in cellular functions and structure, ultimately resulting in death, prompting researchers to study the underlying mechanisms.
  • Utilizing standard and Nanopore RNA sequencing techniques, the study identified numerous novel isoforms and age-related changes in RNA splicing and editing processes in older organisms.
  • The findings highlight a decrease in RNA processing accuracy and an increase in specific RNA modifications, suggesting that these transcriptomic changes contribute to altered gene expression and regulation as organisms age.
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MicroRNAs (miRNAs) regulate gene expression by base-pairing to target sequences in messenger RNAs (mRNAs) and recruiting factors that induce translational repression and mRNA decay. In animals, nucleotides 2-8 at the 5' end of the miRNA, called the seed region, are often necessary and sometimes sufficient for functional target interactions. MiRNAs that contain identical seed sequences are grouped into families where individual members have the potential to share targets and act redundantly.

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Argonaute (AGO) proteins partner with microRNAs (miRNAs) to target specific genes for post-transcriptional regulation. During larval development in Caenorhabditis elegans, Argonaute-Like Gene 1 (ALG-1) is the primary mediator of the miRNA pathway, while the related ALG-2 protein is largely dispensable. Here we show that in adult C.

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