US2014296500A1PendingUtilityA1

Methods and Compositions of Nucleic Acid Ligands for Detection of Clinical Analytes Related to Human Health

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Assignee: BRUNO JOHNPriority: Nov 30, 2010Filed: Feb 25, 2014Published: Oct 2, 2014
Est. expiryNov 30, 2030(~4.4 yrs left)· nominal 20-yr term from priority
Inventors:John G. Bruno
G01N 33/5308G01N 2333/4737G01N 2333/54G01N 33/82C12N 15/115G01N 33/6887G01N 2333/5412G01N 33/66G01N 2333/4712G01N 2333/61
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Abstract

Specific DNA sequences for binding various clinically relevant analytes from the human body are described. Each of these sequences or their linear, two- and three-dimensional linked sequences can function in varying assay and sensor formats with varying degrees of success. Linkage of the whole or partial DNA sequences (putative binding sites) can be used to enhance specificity and affinity towards complex targets, thereby improving assay selectivity and sensitivity in many instances. In addition, a FRET-based quantitative method is described for normalizing analyte data by assessing urine creatinine and urea levels. Finally, a method is described for removing creatinine or urea by size-exclusion chromatography prior to a FRET-based aptamer assay to avoid the denaturing effects of these compounds.

Claims

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1 . A DNA ligand sequence consisting of SEQ ID NO.: 4. 
     
     
         2 . A DNA ligand sequence consisting of SEQ ID NO.: 434. 
     
     
         3 . A DNA ligand sequence consisting of SEQ ID No.: 462.

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