Biologists have long used model organisms to study human diseases, particularly when the model bears a close resemblance to the disease. We present a method that quantitatively and systematically identifies nonobvious equivalences between mutant phenotypes in different species, based on overlapping sets of orthologous genes from human, mouse, yeast, worm, and plant (212,542 gene-phenotype associations). These orthologous phenotypes, or phenologs, predict unique genes associated with diseases. Our method suggests a yeast model for angiogenesis defects, a worm model for breast cancer, mouse models of autism, and a plant model for the neural crest defects associated with Waardenburg syndrome, among others. Using these models, we show that SOX13 regulates angiogenesis, and that SEC23IP is a likely Waardenburg gene. Phenologs reveal functionally coherent, evolutionarily conserved gene networks-many predating the plant-animal divergence-capable of identifying candidate disease genes.angiogenesis | bioinformatics | evolution | gene-phenotype associations | homology B iochemical and molecular functions of a given protein are generally conserved between organisms; this observation is fundamental to biological research. For example, in x-ray crystallography studies, one can often choose the organism from which the protein is most easily crystallized to facilitate the study of the protein's biochemical function. On the other hand, even with a conserved gene, disruption of function may give rise to radically different phenotypic outcomes in different species. For example, mutating the human RB1 gene leads to retinoblastoma, a cancer of the retina, yet disrupting the nematode ortholog contributes to ectopic vulvae (1, 2). Thus, although a gene's "molecular" functions are conserved, the "organism-level" functions need not be. When a conserved gene is mutated, the resulting organism-level phenotype is an emergent property of the system. This bedrock principle underlying the use of model organisms not only allows us to study important aspects of human biology using mice or frogs, but also permits exploration of inherently multicellular processes, such as cancer, using unicellular organisms like yeast.Within this paradigm, once a molecular function has been discovered in one organism, it should be predictable in other organisms: GSK3 homologs in yeast are kinases, and such GSK3 homologs in every other organism will generally be kinases. In contrast, the emergent organism-level phenotypes are far less predictable between organisms, in part because relationships between genes and phenotypes are many-to-many. Manipulation of GSK3 perturbs nutrient and stress signaling in yeast, anteroposterior patterning and segmentation in insects, dorsoventral patterning in frogs, and craniofacial morphogenesis in mice (3-5). Recognizing functionally equivalent organism-level phenotypes between model organisms can therefore be nonobvious, especially across large evolutionary distances.However, the ability to recognize equivalent phenotypes betwee...
