Demo corpus. Scores are computed on a select set of biomedical paper/datasets and may be inaccurate for papers outside this corpus — DataRank relies on network effects that improve with scale. We aim to expand this into a fully open resource pending additional funding.

RAD52-INDEPENDENT MITOTIC GENE CONVERSION IN SACCHAROMYCES CEREVISIAE FREQUENTLY RESULTS IN CHROMOSOMAL LOSS

Genetics(1985)10.1093/genetics/111.1.7Source: DataRank Database

RAD52-INDEPENDENT MITOTIC GENE CONVERSION IN SACCHAROMYCES CEREVISIAE FREQUENTLY RESULTS IN CHROMOSOMAL LOSS is a research paper published in Genetics (1985). On theSindex it has a DataRank of 4.8. It has been cited 91 times, with 76 citing works in its 1-hop citation network.

N/A

4.8DataRank · unranked

4.8

91 citations · base score 4.5

Cite:

datarank_citation_only_1hop_v6· scope data_onlyMethodology

Abstract

ABSTRACT We have examined spontaneous, interchromosomal mitotic recombination events between his4 alleles in both Rad+ and rad52 strains of Saccharomyces cerevisiae. In Rad+ strains, 74% of the His+ prototrophs resulted from gene conversion events without exchange of flanking markers. In diploids homozygous for the rad52-1 mutation, the frequency of His+ prototroph formation was less than 5% of the wild-type value, and more than 80% of the gene conversion events were accompanied by an exchange of flanking markers. Most of the rad52 intragenic recombination events arose by gene conversion accompanied by an exchange of flanking markers and not by a simple reciprocal exchange between the his4A and his4C alleles. There were also profound effects on the kinds of recombinant products that were recovered. The most striking effect was that RAD52-independent mitotic recombination frequently results in the loss of one of the two chromosomes participating in the gene conversion event.

›Data sources & pipeline

Pipeline:MetadataData-paper checkEnrichmentCitation networkScoring

Enrichment:Pending

FAIR Checklist

Context only (not used in score)

Findable (1/2)

Has DOI

Accessible (0/2)

Interoperable (0/2)

Reusable (0/3)

FAIR checklist signals are shown for context only and do not affect DataRank scoring.

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DataRank Breakdown

Base Score 14%Citation Network 86%

Base Score Contribution

0.678

From this paper's citation signal

Citation Network Contribution

4.1

From 71 citing papers with measurable signal

Learn more about DataRank methodology →

Top 3 citers driving the network score

Ranked by citation count — the same ordering the engine uses when summing log1p(C_q) over citers.

Role ofRAD52Epistasis Group Genes in Homologous Recombination and Double-Strand Break Repair
Microbiology and Molecular Biology Reviews2002970 citationsDataRank 15.8
Rad52 Promotes Postinvasion Steps of Meiotic Double-Strand-Break Repair
Molecular Cell2008122 citationsDataRank 4.8
Genetic control of RNA polymerase I-stimulated recombination in yeast.
Genetics199035 citationsDataRank 2.6

Why this DataRank?

DataRank blends this paper's own citation count with the influence of the papers that cite it. Here, roughly 14% comes from its base citations and 86% from the citation network (71 citing papers contributed measurable signal).

Base score B(p): log1p(citation_count) — grows sub-linearly, so a paper with 1,000 citations is not 10× a paper with 100.
Network N(p): Σ over citers of log1p(C_q) ÷ max(outdegree_q, 1). Being cited by a highly-cited paper with few references counts most.
Damping factor d = 0.85: DataRank = (1−d)·B(p) + d·N(p) — the two cards above are each already multiplied by their share.
Self-citations excluded: Citers sharing any OpenAlex author ID with this paper are filtered out before the network sum.

Citers are pulled from OpenAlex sorted by cited_by_count:descand capped per paper, so when the cap binds we keep the highest-signal references and the score is reproducible across reruns.

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Node colors:CenterData PaperData + Open AccessNon-dataSelected & links| Node size = percentile rank