1.Optimizing the host bacteria to make a large naive phage antibody library in the recombination system.
Wei SUN ; Heng LIN ; Fang HUA ; Zhuo-Wei HU
Acta Pharmaceutica Sinica 2013;48(1):66-70
To prepare large naive phage antibody library, the host bacteria with high transformation efficiency is used in the Cre-LoxP recombination system. The variable regions of immunoglobulin light and heavy genes were amplified from lymphocytes collected from adult peripheral blood and newborn cord blood. The genes were spliced to form the single-chain variable fragments (scFv) by overlap PCR, cloned into pDAN5a vector and then transformed into XL2-blue MRF' with the Hte gene. Compared with XL1-blue strain, the size of the primary library was increased by 3.9 times. The primary library infected Cre recombinase-expressing bacteria, and the genes between phagemids created many new VH/VL combinations. The library was calculated to have a diversity of 1.7 x 10(11) and validated by the selection of antibodies against six different protein antigens. This library provides the basis for further selection of antibody-based drugs. It is the first time to report that XL2-blue MRF' can be used to improve the diversity of the library in the recombination system.
Adult
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Escherichia coli
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genetics
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immunology
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Genetic Vectors
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Humans
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Immunoglobulin Heavy Chains
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genetics
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Immunoglobulin Light Chains
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genetics
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Immunoglobulin Variable Region
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genetics
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Infant, Newborn
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Integrases
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metabolism
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Lymphocytes
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immunology
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Peptide Library
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Recombination, Genetic
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genetics
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Single-Chain Antibodies
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genetics
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metabolism
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Transformation, Genetic
2.Development of thymic lymphomas in mice disrupted of Brca2 allele in the thymus.
Experimental & Molecular Medicine 2008;40(3):339-344
Germ-line mutations in BRCA2 predispose to early-onset cancer. Homozygous mutant mouse, which has Brca2 truncated in exon 11 exhibit paradoxic occurrence of growth retardation and development of thymic lymphomas. However, due to its large embryonic lethality, cohort studies on the thymic lymphomas were not feasible. With the aid of Cre-loxP system, we demonstrate here that thymus-specific disruption of Brca2 allele without crossing it to p53-mutant background leads to the development of thymic lymphomas. Varying from 16 weeks to 66 weeks after birth, 25% of mice disrupted of Brca2 in the thymus died of thymic lymphomas, whereas previous report did not observe lymphomagenesis using similar Cre-loxP system. Future analysis of thymic lymphomas from these mice presented here will provide information on the cooperative mutations that are required for the BRCA2-associated pathogenesis of cancer.
Animals
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BRCA2 Protein/deficiency/*genetics
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CD4-CD8 Ratio
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Cell Separation
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Flow Cytometry
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Integrases/*genetics/immunology
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Lymphoma/*genetics/immunology/metabolism/pathology
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Mice
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Mice, Knockout
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Organ Specificity
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*Sequence Deletion
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T-Lymphocytes/enzymology/*immunology
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Thymus Gland/immunology/metabolism/pathology
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Thymus Neoplasms/*genetics/immunology/metabolism/pathology
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Tumor Suppressor Protein p53/deficiency/genetics/immunology