Transgenic model for delay-type hypersensitivity (DTH) and use thereof

What is claimed is: 1. A homozygous IKK-β C46A transgenic, knock-in, C57BL/6J mouse whose genome comprises a transgene encoding a single cysteine-to-alanine mutation at position 46 (C46A) in the endogenous amino acid sequence of SEQ ID NO:2, wherein the transgenic mouse comprises kidney tissues with a stronger in vivo kinase activity of IKK-β and ear tissues with an enhanced in vivo inflammatory response to a delay-type hypersensitivity (DTH)-inducing agent relative to an equal amount of the respective tissues from a C57BL/6J wild-type mouse. 2. A method of preparing the homozygous IKK-β C46A transgenic, knock-in, C57BL/6J mouse of claim 1 , said method comprising: (a) transfecting mouse embryonic stem cells by electroporating with a linearized targeting construct with Neo selection gene, wherein said targeting construct is IKK-β C46A targeting construct comprising the nucleotide sequence of SEQ ID NO: 1; (b) identifying and selecting recombinant embryonic stem cells obtained from step (a) that have undergone correct homologous recombination; (c) injecting recombinant embryonic stem cells from step (b) into blastocysts; (d) transplanting blastocysts obtained from step (c) into a pseudopregnant mouse to generate chimeric IKK-β C46A mice; (e) mating chimeric IKK-β C46A males obtained from step (d) with C57BL/6J females to produce heterologous IKK-β C46A transgenic, knock-in, C57BL/6J mice; and (f) mating heterologous IKK-β C46A transgenic, knock-in, C57BL/6J mice obtained from step (e) to produce homozygous IKK-β C46A transgenic, knock-in, C57BL/6J mouse of claim 1 . 3. The method of claim 2 , wherein the targeting construct being a template to introduce a single point mutation at the cysteine (C) residue at position 46 in the endogenous amino acid sequence of SEQ ID NO:2 being replaced by alanine (A). 4. The method of claim 2 , wherein said recombinant embryonic stem cells are further validated by PCR and gene sequencing using two pairs of forward and reverse primers having SEQ ID NO: 3, SEQ ID NO: 4, SEQ ID NO: 5, and SEQ ID NO: 6. 5. The method of claim 2 , wherein said linearized targeting construct contains homology arms of 3.8 kb at 5′ arm and 2.5 kb at 3′ arm, said homology arms being constructed by PCR using five pairs of forward and reverse primers comprising SEQ ID NOs: 7 to 16. 6. The method of claim 4 , wherein the forward and reverse primer pairs having SEQ ID No: 3 and SEQ ID NO: 4 are used to evaluate 5′arm of the genes expressing IKK-β C46A mutant for genotyping. 7. The method of claim 4 , wherein the forward and reverse primer pairs having SEQ ID NO: 5, and SEQ ID NO: 6 are used to evaluate 3′arm of the genes expressing IKK-β mutant for genotyping. 8. A method for determining therapeutic or prophylactic activity of a test compound in delay-type hypersensitivity (DTH) and other inflammatory or cancerous diseases mediated by activation of IKK-β C46A mutant protein comprising: (a) administering said test compound to the transgenic C57BL/6J mouse of claim 1 ; (b) measuring one or more physiological, morphological, molecular and/or histological parameter(s); and (c) comparing the measure in (b) with a measure obtained from a control mouse to observe or analyze any difference between two measures qualitatively and quantitatively in order to determine whether the test compound administered is specific and effective for treating or prophylaxing DTH and other inflammatory or cancerous diseases mediated by activation of IKK-β C46A mutant, protein. 9. The method of claim 8 , wherein the test compound specifically binds to cysteine 46 residue of the IKK-β protein in the epithelial cell in order to inhibit IKK-β and NF-κB signaling, wherein an activation of said signaling potentially leads to severe inflammatory response or cancerous diseases; otherwise, if the test compound can target IKK-β via other binding sites but not on cysteine 46 residue, the activation of IKK-β C46A and NF-κB signaling pathway can be suppressed. 10. The method of claim 8 , wherein the inflammatory or cancerous diseases are selected from a group consisting of arthritis, delay-type hypersensitivity autoimmune disease and various types of cancer with different origin mediated by activation of IKK-β C46A mutant protein.