Complete replacement of mitochondrial DNA in Drosophila

The introduction of foreign mitochondria or mitochondrial DNA into a cell is a useful technique for clarifying the molecular mechanisms responsible for the maintenance of mitochondria. Novel combinations of mitochondrial and nuclear genomes have been studied in mammalian cells in culture and in yeast. In Drosophila, we have recently constructed heteroplasmic flies possessing both endogenous mitochondrial DNA and foreign mitochondrial DNA by intra- and interspecific transplantation of germ plasm. During the maintenance of these heteroplasmic lines, flies of D. melanogaster are produced that no longer possess their own mitochondrial DNA but retain the foreign mitochondrial DNA from D. mauritiana. .These flies are fertile and the foreign mitochondrial DNA is stably maintained in their offspring. Here we report the complete replacement of endogenous mitochondrial DNA with that from another multicellular species. Molecular and genetic analysis of this replacement in Drosophila should provide new insight into the functional interaction between nuclear and organelle genomes.     

Unique allelic restriction fragments of the human Ha-ras locus in leukocyte and tumour DNAs of cancer patients

White blood cell DNA from cancer patients and DNA from tumours and tumour-derived cell lines frequently demonstrated allelic restriction fragments of the Harvey ras oncogene locus not found in the unaffected population. The presence of such unusual alleles may be linked to susceptibility to cancer.     

中国白兔线粒体DNA限制性图谱

用 ６ 种限制性内切酶分析了中国白兔的线粒体 Ｄ Ｎ Ａ（ｍ ｔ Ｄ Ｎ Ａ）。测得其相对分子质量约为１６．８, Ｅｃｏ ＲⅤ, Ｂａｍ ＨⅠ, ＰｓｔⅠ, Ｅｃｏ ＲⅠ, ＨｉｎｄⅢ在中国白兔 ｍ ｔ Ｄ Ｎ Ａ 上分别有 １,２,２,２,６ 个切点, ＳａｌⅠ 在其上没有切点。根据单酶降解和双酶降解片段的相对分子质量,构建了中国白兔ｍ ｔ Ｄ Ｎ Ａ的限制性内切酶图谱。     

Molecular and phenotypic variation in the achaete-scute region of Drosophila melanogaster

Variation in quantitative characters underlies much adaptive evolution and provides the basis for selective improvement of domestic species, yet the genetic nature of quantitative variation is poorly understood. Many loci affecting quantitative traits have been identified by the segregation of mutant alleles with major qualitative effects. These alleles may represent an extreme of a continuum of allelic effects, and most quantitative variation could result from the segregation of alleles with subtle effects at loci identified by alleles with major effects. The achaete-scute complex in Drosophila melanogaster plays a central part in bristle development and has been characterized at the molecular level. The hypothesis that naturally occurring quantitative variation in bristle number could be associated with wild-type alleles of achaete-scute was tested by correlating phenotypic variation in bristle number with molecular variation in restriction maps in this region among chromosomes extracted from natural populations. DNA insertion variation in the achaete-scute region was found to be strongly associated with variation in bristle number.     

A zone of non-proliferating cells at a lineage restriction boundary in Drosophila

The use of X-ray-induced mitotic recombination to genetically mark individual cells and their descendants during development has led to the discovery of lineage restriction boundaries in Drosophila imaginal disks, dividing the disks into areas called compartments. Clones of cells initiated after a given developmental stage are unable to grow across these boundaries, even if provided with a growth rate advantage over the remaining cells. It has been suggested that cells within compartments are distinguished by the differential activation of selector genes and that the lineage restrictions are maintained by adhesivity differences between the cells in different compartments, but other mechanisms have not been ruled out. Recently a discrete population of cells with unusual permeability properties has been described along an intersegmental lineage restriction boundary in Oncopeltus, suggesting that a lineage restriction could be maintained by a zone of cells which present a barrier to clone growth. Here we demonstrate by autoradiography the presence of a narrow zone of non-proliferating cells (ZNC) coincident with the presumptive wing margin in the Drosophila wing disk, and suggest that this could account for the observed lineage restriction between presumptive dorsal and ventral surfaces of the wing. As the anterior/posterior compartment boundary does not coincide with a ZNC, the results indicate that different lineage boundaries may be maintained by different mechanisms.     

瓢虫DNA的提取研究

对鞘翅目瓢虫科昆虫的基因组ＤＮＡ进行了提取，经紫外透射分析仪检测，ＤＮＡ带子整齐；又经蛋白质核酸分析仪测定，ＯＤ值在１．６～１．８的样品占６２．５％，其余均接近这种纯度．这种ＤＮＡ提取方法对瓢虫的新鲜标本、酒精浸泡标本及干制标本均有较好的效果．     

Drosophila melanogaster mitochondrial DNA, a novel organization and genetic code

The sequence of a 4,869 base-pair fragment of Drosophila melanogaster mitochondrial DNA is presented. It contains genes for cytochrome oxidase subunits I, II and III, ATPase subunit 6 and six tRNAs together with two unassigned reading frames. The gene organization differs from that of mammalian mitochondrial DNAs. Evidence is provided for a genetic code in which AGA codes for serine and the quadruplet ATAA is used in initiation of translation.     

Drosophila pink1 is required for mitochondrial function and interacts genetically with parkin

Parkinson's disease is the second most common neurodegenerative disorder and is characterized by the degeneration of dopaminergic neurons in the substantia nigra. Mitochondrial dysfunction has been implicated as an important trigger for Parkinson's disease-like pathogenesis because exposure to environmental mitochondrial toxins leads to Parkinson's disease-like pathology. Recently, multiple genes mediating familial forms of Parkinson's disease have been identified, including PTEN-induced kinase 1 (PINK1; PARK6) and parkin (PARK2), which are also associated with sporadic forms of Parkinson's disease. PINK1 encodes a putative serine/threonine kinase with a mitochondrial targeting sequence. So far, no in vivo studies have been reported for pink1 in any model system. Here we show that removal of Drosophila PINK1 homologue (CG4523; hereafter called pink1) function results in male sterility, apoptotic muscle degeneration, defects in mitochondrial morphology and increased sensitivity to multiple stresses including oxidative stress. Pink1 localizes to mitochondria, and mitochondrial cristae are fragmented in pink1 mutants. Expression of human PINK1 in the Drosophila testes restores male fertility and normal mitochondrial morphology in a portion of pink1 mutants, demonstrating functional conservation between human and Drosophila Pink1. Loss of Drosophila parkin shows phenotypes similar to loss of pink1 function. Notably, overexpression of parkin rescues the male sterility and mitochondrial morphology defects of pink1 mutants, whereas double mutants removing both pink1 and parkin function show muscle phenotypes identical to those observed in either mutant alone. These observations suggest that pink1 and parkin function, at least in part, in the same pathway, with pink1 functioning upstream of parkin. The role of the pink1-parkin pathway in regulating mitochondrial function underscores the importance of mitochondrial dysfunction as a central mechanism of Parkinson's disease pathogenesis.