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1. DNA and RNA base editors can correct the majority of pathogenic single nucleotide variants.

2. Temporal genomic analysis of melanoma rejection identifies regulators of tumor immune evasion.

3. Antibody interfaces revealed through structural mining.

4. Cross-species identification of cancer resistance-associated genes that may mediate human cancer risk.

5. Synthetic lethality-based prediction of anti-SARS-CoV-2 targets.

6. Genome-scale metabolic modeling reveals SARS-CoV-2-induced metabolic changes and antiviral targets.

7. Synthetic lethality-based prediction of anti-SARS-CoV-2 targets.

8. Genome-scale metabolic modeling reveals SARS-CoV-2-induced metabolic changes and antiviral targets.

9. Matching whole genomes to rare genetic disorders: Identification of potential causative variants using phenotype-weighted knowledge in the CAGI SickKids5 clinical genomes challenge.

10. Assessment of patient clinical descriptions and pathogenic variants from gene panel sequences in the CAGI-5 intellectual disability challenge.

11. Reports from the fifth edition of CAGI: The Critical Assessment of Genome Interpretation.

12. Assessment of predicted enzymatic activity of α-N-acetylglucosaminidase variants of unknown significance for CAGI 2016.

13. CAGI SickKids challenges: Assessment of phenotype and variant predictions derived from clinical and genomic data of children with undiagnosed diseases.

14. Predicting venous thromboembolism risk from exomes in the Critical Assessment of Genome Interpretation (CAGI) challenges.

15. Assessing computational predictions of the phenotypic effect of cystathionine-beta-synthase variants.

16. Assessing the performance of in silico methods for predicting the pathogenicity of variants in the gene CHEK2, among Hispanic females with breast cancer.

17. Assessment of methods for predicting the effects of PTEN and TPMT protein variants.

18. Harnessing formal concepts of biological mechanism to analyze human disease.

20. Determination of disease phenotypes and pathogenic variants from exome sequence data in the CAGI 4 gene panel challenge.

21. Ensemble variant interpretation methods to predict enzyme activity and assign pathogenicity in the CAGI4 NAGLU (Human N-acetyl-glucosaminidase) and UBE2I (Human SUMO-ligase) challenges.

22. CAGI4 SickKids clinical genomes challenge: A pipeline for identifying pathogenic variants.

23. CAGI4 Crohn's exome challenge: Marker SNP versus exome variant models for assigning risk of Crohn disease.

24. Matching phenotypes to whole genomes: Lessons learned from four iterations of the personal genome project community challenges.

25. Performance of in silico tools for the evaluation of p16INK4a (CDKN2A) variants in CAGI.

26. Lessons from the CAGI-4 Hopkins clinical panel challenge.

27. Working toward precision medicine: Predicting phenotypes from exomes in the Critical Assessment of Genome Interpretation (CAGI) challenges.

28. Consensus Genome-Wide Expression Quantitative Trait Loci and Their Relationship with Human Complex Trait Disease.

29. Genetic Basis of Common Human Disease: Insight into the Role of Missense SNPs from Genome-Wide Association Studies.

30. Insights from GWAS: emerging landscape of mechanisms underlying complex trait disease.

31. Protein characterization of a candidate mechanism SNP for Crohn's disease: the macrophage stimulating protein R689C substitution.

32. Structural insights into the substrate binding and stereoselectivity of giardia fructose-1,6-bisphosphate aldolase.

33. A top-down approach to infer and compare domain-domain interactions across eight model organisms.

34. Tracing the origin of functional and conserved domains in the human proteome: implications for protein evolution at the modular level.

35. DMAPS: a database of multiple alignments for protein structures.

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