疏水吸附分离酵母 S.Cerevisiae 中的 L-天门冬氨酸酶的研究(英文)

研究了疏水柱吸附分离工业酵母（Ｓ．Ｃｅｒｅｖｉｓｉａｅ）中的Ｌ－天门冬氨酸酶．考察了三种疏水吸附剂ＴｓｋｇｅｌＢｕｔｙ＿Ｔｏｙｏｐｅａｒｌ,ＴｓｋｇｅｌＰｈｅｎｙｌ＿Ｔｏｙｏｐｅａｒｌ和ＴｓＫｇｅｌＥｔｈｅｒ＿Ｔｏｙｏｐｅａｒｌ６５０Ｃ的吸附性能．研究表明,通过选择控制流动相的ｐＨ值和离子强度,一次吸附过程中Ｌ－天门冬氨酸酶的分离纯化纯度可提高１４倍并保持较高的活性。实验还考察了吸附等温线类型和温度等因素的影响．结果表明,酵母中分子的电荷和疏水性是疏水柱吸附的重要影响因素．     

The NCBI dbGaP database of genotypes and phenotypes

The National Center for Biotechnology Information has created the dbGaP public repository for individual-level phenotype, exposure, genotype and sequence data and the associations between them. dbGaP assigns stable, unique identifiers to studies and subsets of information from those studies, including documents, individual phenotypic variables, tables of trait data, sets of genotype data, computed phenotype-genotype associations, and groups of study subjects who have given similar consents for use of their data.     

未澄清酵母均化液中 L-天门冬氨酸酶的分离——疏水膨胀床直接吸附法(英文)

研究了用疏水膨胀床直接从未澄清酵母（Ｓ．ｃｅｒｅｖｉｓｉａｅ）均化液中分离Ｌ－天门冬氨酸酶的过程．吸附和冲洗采用膨胀床模式,而酶的洗提采用沉降床模式．在适当的疏水条件下,膨胀床中的疏水吸附剂（ＴｓｋｇｅｌＰｈｅｎｙｌ＿Ｔｏｙｏｐｅａｒｌ６５０Ｃ）可从未澄清均化液中直接捕集分离Ｌ－天门冬氨酸酶．通过梯度洗提,一次膨胀床吸附过程中,酶活的洗脱率为９５％,均化液中酶的总回收率为６５％,洗脱液纯度为１３倍．本方法将膨胀床和疏水性吸附的特长有机地结合起来,是生物活性蛋白酶分离纯化的一个重要手段．     

C-terminal truncations in human 3'-5' DNA exonuclease TREX1 cause autosomal dominant retinal vasculopathy with cerebral leukodystrophy

Autosomal dominant retinal vasculopathy with cerebral leukodystrophy is a microvascular endotheliopathy with middle-age onset. In nine families, we identified heterozygous C-terminal frameshift mutations in TREX1, which encodes a 3'-5' exonuclease. These truncated proteins retain exonuclease activity but lose normal perinuclear localization. These data have implications for the maintenance of vascular integrity in the degenerative cerebral microangiopathies leading to stroke and dementias.     

Cell fusion is the principal source of bone-marrow-derived hepatocytes

Evidence suggests that haematopoietic stem cells might have unexpected developmental plasticity, highlighting therapeutic potential. For example, bone-marrow-derived hepatocytes can repopulate the liver of mice with fumarylacetoacetate hydrolase deficiency and correct their liver disease. To determine the underlying mechanism in this murine model, we performed serial transplantation of bone-marrow-derived hepatocytes. Here we show by Southern blot analysis that the repopulating hepatocytes in the liver were heterozygous for alleles unique to the donor marrow, in contrast to the original homozygous donor cells. Furthermore, cytogenetic analysis of hepatocytes transplanted from female donor mice into male recipients demonstrated 80,XXXY (diploid to diploid fusion) and 120,XXXXYY (diploid to tetraploid fusion) karyotypes, indicative of fusion between donor and host cells. We conclude that hepatocytes derived form bone marrow arise from cell fusion and not by differentiation of haematopoietic stem cells.