Project description:The Human Proteome Project currently seeks to understand the complexities of functional genomics and proteomics and to systematically identify and functionally characterize noncanonical translated sequences, such as micropeptides, will enrich the understanding of the human genome. By producing a high-coverage micropeptide sequencing reference library with 11,931,202 open reading frames and devising an alternative ultrafiltration-concentrated tandem mass spectrometry assay, we effectively confirmed 10,771 unlabeled proteins. Nearly 40% of them were derived from noncoding RNAs, suggesting that there may be a large number of misannotations in the human genome. These micropeptides exhibited abundance at subcellular locations and broad gastric cancer relevance. CRISPR screening showed that 1161 candidates had critical growth regulatory functions that were associated with their genetic properties. Excitingly, shorter sequenced micropeptides exhibited natural peptide-based drug potential or strong carcinogenic effects. Our findings illustrate a hitherto unrecognized micropeptidome and highlight its valuable implications for cancer therapy and drug development.

Project description:The Human Proteome Project currently seeks to understand the complexities of functional genomics and proteomics and to systematically identify and functionally characterize noncanonical translated sequences, such as micropeptides, will enrich the understanding of the human genome. By producing a high-coverage micropeptide sequencing reference library with 11,931,202 open reading frames and devising an alternative ultrafiltration-concentrated tandem mass spectrometry assay, we effectively confirmed 10,771 unlabeled proteins. Nearly 40% of them were derived from noncoding RNAs, suggesting that there may be a large number of misannotations in the human genome. These micropeptides exhibited abundance at subcellular locations and broad gastric cancer relevance. CRISPR screening showed that 1161 candidates had critical growth regulatory functions that were associated with their genetic properties. Excitingly, shorter sequenced micropeptides exhibited natural peptide-based drug potential or strong carcinogenic effects. Our findings illustrate a hitherto unrecognized micropeptidome and highlight its valuable implications for cancer therapy and drug development.

Project description:TGF-β signaling is a central regulator of early development in metazoans, yet our understanding of the scope of TGF-β signaling’s downstream targets and associated physiological mechanisms in specifying developmentally appropriate cell fates is far from complete. Here, we found that a highly conserved, primitive-streak-specific micropeptide is a direct target of TGF-b/Nodal signaling. This transmembrane micropeptide (NEMEP) is essential for mesendoderm differentiation. Depletion of NEMEP impaired mesendoderm differentiation and caused a significant decrease in glucose uptake, while TGF-β signaling enhances glucose uptake in a NEMEP-dependent manner. Biochemically, we show that NEMEP promotes glucose uptake through its interactions with GLUT1/3. Thus, beyond expanding the scope of known TGF-β signaling targets in early development and showing that this target micropeptide augments the glucose uptake function of major glucose transporters during mesendoderm differentiation, our study provides a clear example for the direct functional impact of altered metabolism on cell fate determination in early embryogenesis.

Project description:A cardiac fibroblast-enriched micropeptide regulates inflammation

Project description:In this study, we generated nucleotide-resolution translatome as well as transcriptome data of isolated primary cardiomyocytes undergoing hypertrophy. More than 10,000 open reading frames (ORF) were detected from the deep sequencing of ribosome protected fragments orchestrating the shift of translatome in hypertrophied cardiomyocytes.We further identified more than 100 potential micropeptides encoded by uncharacterized small open reading frames (sORFs) in the long noncoding RNA genes. Over two-thirds of these micropeptide candidates were experimentally validated in a random test with three micropeptides showing regulatory function in cardiomyocyte hypertrophy via modulating the activities of Oxidative phosphorylation, Calcium signaling pathway, and MAPK signaling pathway.Our study provided a genome-wide overview of the translational controls of cardiomyocyte hypertrophy and demonstrated an unrecognized role of micropeptides in cardiomyocyte biology.

Project description:In this study, we generated nucleotide-resolution translatome as well as transcriptome data of isolated primary cardiomyocytes undergoing hypertrophy. More than 10,000 open reading frames (ORF) were detected from the deep sequencing of ribosome protected fragments orchestrating the shift of translatome in hypertrophied cardiomyocytes.We further identified more than 100 potential micropeptides encoded by uncharacterized small open reading frames (sORFs) in the long noncoding RNA genes. Over two-thirds of these micropeptide candidates were experimentally validated in a random test with three micropeptides showing regulatory function in cardiomyocyte hypertrophy via modulating the activities of Oxidative phosphorylation, Calcium signaling pathway, and MAPK signaling pathway.Our study provided a genome-wide overview of the translational controls of cardiomyocyte hypertrophy and demonstrated an unrecognized role of micropeptides in cardiomyocyte biology.

Project description:In this study, we generated nucleotide-resolution translatome as well as transcriptome data of isolated primary cardiomyocytes undergoing hypertrophy. More than 10,000 open reading frames (ORF) were detected from the deep sequencing of ribosome protected fragments orchestrating the shift of translatome in hypertrophied cardiomyocytes.We further identified more than 100 potential micropeptides encoded by uncharacterized small open reading frames (sORFs) in the long noncoding RNA genes. Over two-thirds of these micropeptide candidates were experimentally validated in a random test with three micropeptides showing regulatory function in cardiomyocyte hypertrophy via modulating the activities of Oxidative phosphorylation, Calcium signaling pathway, and MAPK signaling pathway.Our study provided a genome-wide overview of the translational controls of cardiomyocyte hypertrophy and demonstrated an unrecognized role of micropeptides in cardiomyocyte biology.

Project description:Functional micropeptides embedded within RNA transcripts previously classified as noncoding may play significant roles in lung tumorigenesis that remain largely unexplored. By integrating ribosome sequencing and mass spectrometry data, we identified a 46-amino-acid oncogenic micropeptide encoded by the lncRNA DSP-AS1, which we have named Translation Initiation Activated Micropeptide (TIAMP), in lung adenocarcinoma (LUAD). TIAMP is aberrantly overexpressed in LUAD and is associated with poor prognosis. Its oncogenic effects—including enhanced proliferation, survival, and invasiveness—were confirmed in both in vitro and in vivo models. TIAMP colocalizes with the translation machinery and orchestrates translational reprogramming by selectively promoting the translation of mRNAs encoding oncogenic factors in LUAD. Mechanistically, TIAMP binds to both eIF4G, a cap-binding subunit, and YTHDF1, an m6A reader that recruits eIF3 to methylated mRNAs, thereby forming a "closed loop" between YTHDF1 and eIF4G. This interaction positions YTHDF1 in proximity to the translation initiation complex, facilitating the efficient loading of the 40S ribosomal subunit onto target mRNAs. Targeting TIAMP yields significant anticancer effects both in vitro and in vivo. Our findings uncover the oncogenic role of this previously uncharacterized micropeptide in orchestrating mRNA translation, providing a compelling rationale for the development of anti-LUAD therapies targeting the translation machinery.

Project description:Probing condensate microenvironments and functions with a micropeptide “killswitch”

Project description:A fundamental goal of genomics is to identify the complete set of expressed proteins. Automated annotation strategies rely on assumptions about protein-coding sequences (CDSs), e.g., they are conserved, do not overlap, and exceed a minimum length. However, an increasing number of newly discovered proteins violate these rules. Here we present an experimental and analytical framework, based on ribosome profiling and linear regression, for systematic identification and quantification of translation. Application of this approach to lipopolysaccharide-stimulated mouse dendritic cells and HCMV-infected human fibroblasts identifies thousands of novel CDSs, including micropeptides and variants of known proteins, that bear the hallmarks of canonical translation and exhibit comparable translation levels and dynamics to annotated CDSs. Remarkably, many translation events are identified in both mouse and human cells even when the peptide sequence is not conserved. Our work thus reveals an unexpected complexity to mammalian translation suited to provide both conserved regulatory or protein-based functions. 37 ribosome footprint samples from mouse BMDCs across a time course of LPS stimulation and in the presence or absence of translation inhibitors cycloheximide, harringtonine, or lactimidomycin. A mock (non-LPS stimulated) time course is also included, collected in the presence of cycloheximide. Two replicates are available for the LPS timecourse under CHX treatment.