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     Quick Explanation



    Author review β€” Han Altae-Tran (concise)

    Altae-Tran is a productive computational/experimental researcher whose work on RNA-guided nucleases, compact RNA editors, and computational methods has high impact (multiple Science/Nature/Nat Biotech papers) and broad citations across 2013–2025 and Nature/Cell/NatBiotech articles




     Long Explanation



    Author Review: Han Altae-Tran β€” Evidence-based critique & visualization

    Visual summary (citations & output over time)

    Plot: cited-by counts per calendar year from OpenAlex summary (counts_by_year provided in author metadata).

    Core evidence & representative high-impact works

    • High-impact first/senior-authored contributions to discovery of programmable RNA-guided endonucleases in widespread transposons (Science 2021), with experimental validation and evolutionary analysis
    • Author in Nature 2023 describing Fanzor β€” a eukaryotic programmable RNA-guided endonuclease β€” demonstrating cross-domain discoveries and experimental structural/functional work
    • Multiple contributions to compact RNA editors and CRISPR-related tool development in high-profile journals (Nat Biotech 2021; Cell 2021) indicating translational and methodological breadth

    Author metrics (provided sources)

    Microsoft Academic/semantic scholar style summary provided: h-index β‰ˆ 17, total citations β‰ˆ 1,766, paper count β‰ˆ 25 (paper list provided).

    OpenAlex record (aggregated): works_count = 38, cited_by_count = 4,434, h_index = 22 (counts_by_year shown in plot above) β€” indicating broader coverage in OpenAlex aggregation.

    Note: different indexing sources (author-supplied list vs OpenAlex) yield different totals; OpenAlex aggregates more works and citations, raising h-index and cited_by_count compared with earlier snapshot.

    Scientific strengths

    • High-impact, field-changing contributions (Science/Nature/Nat Biotech/Cell coauthorship and lead authorship) showing discovery + experimental validation in molecular biology and computational genomics
    • Interdisciplinary skillset β€” computational discovery, structural biology collaborations, and molecular tool engineering (e.g., Fanzor, Cas13, compact editors).
    • Rapid, sustained productivity across 2013–2025 with multiple widely-cited items (OpenAlex: works_count 38; cited_by_count 4,434) suggesting influence and robust citation footprint

    Potential limitations & blindspots

    • Authorship mix: many high-impact items are multi-author collaborations; disentangling individual contribution across computational, experimental, and conceptual roles sometimes requires reading author contribution statements in each paper.
    • Translational maturity: several discoveries (Fanzor, compact editors, TnpB-based systems) are early-stage tool discoveries; broad in vivo safety, target range, and off-target profiling remain to be exhaustively characterized (common limitation for new nuclease tools)
    • Indexing/citation variance: differences between provided paper list and OpenAlex totals highlight the usual bibliometric uncertainty (database coverage, preprints, and name disambiguation affect h-index and citation totals).

    Biases & sources of error to consider in judging the author

    • Publication bias toward positive/novel tool papers (common across genomics/CRISPR literature) β€” important to check negative/failed experiments or replication attempts where available.
    • Collaborative network effects: coauthorship with established groups (e.g., Broad, McGovern) can amplify visibility β€” separate scientific novelty from sociological citation amplification by reading methods and direct contributions.
    • Indexing heterogeneity (OpenAlex vs other indices) β€” reliance on one bibliometric source can misestimate impact; use multiple sources for robust assessment.

    Conclusions (evidence-weighted)

    Altae-Tran is an active, high-impact researcher bridging computational genomics and experimental molecular biology with multiple well-cited discoveries (TnpB/IS200 discovery, Fanzor, compact editors). Evidence shows strong novelty and interdisciplinary strength, with the normal caveats about early-stage tool maturation and bibliometric variability

    What would change this assessment: large-scale independent replication showing poor nuclease specificity or failure to reproduce biochemical results would lower novelty/impact; conversely, robust in vivo demonstrations and tool development would strengthen translational impact.

    Representative citations used in this review



    Feedback:   

    Updated: January 28, 2026

    BGPT Author Review



    Scientific Quality

    80%

    Altae-Tran demonstrates high scientific capability: first/senior authorship on foundational genomic/biochemical discoveries (TnpB, Fanzor), strong interdisciplinary integration (computational genomics + experiments), and a robust citation footprint; minor deductions reflect bibliometric uncertainty and the early translational state of several tool-discovery papers.



    Communication Quality

    80%

    Papers are published in top-tier journals with clear methods and substantial supporting data; exposition and collaborative clarity are generally strong, though some large multi-author works require reading author-contribution details to allocate credit precisely.



    Author Novelty

    90%

    Contributions (discovering new classes of RNA-guided nucleases and eukaryotic Fanzor, compact RNA editors) are novel within CRISPR/evolutionary genomics space; novelty is high because these findings open new mechanistic and tool-development directions.



    Scientific Rigor

    80%

    Work combines genome-scale computational searches, phylogenetics, structural biology, and biochemical validation β€” methods and controls are generally appropriate and detailed; some claims (tool readiness, broad specificity) require further extensive benchmarking and replication.

     Analysis Wizard



    Parsing OpenAlex counts_by_year and plotting citation/time curves to quantify citation trends and compute an approximate per-paper mean citation; useful for bibliometric trend analysis.



     Hypothesis Graveyard



    Hypothesis: TnpB systems are functionally equivalent to Cas9 across eukaryotes β€” rejected because current data show limited biochemical characterization and domain differences reducing direct equivalence.


    Hypothesis: High citation counts guarantee translational readiness β€” unsound because citation reflects interest and novelty, not mature safety/efficacy validation.

     Science Art


    Author Review: Han Raut Altae-Tran Science Art

     Science Movie



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     Discussion








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