financial management
Post has two assignments
1:International financial management
Order Description
The scenario:
The board of directors of a manufacturing company, Green Battery Technology Systems (GBTS Plc), based in the United Kingdom. Your company manufactures batteries used in the manufacture of various types of electric cars. You supply a number of major car producers worldwide, exporting to Germany, China, and the United States. In January 2015 (a year ago), GBTS set up a joint venture with Beijing Battery Power Technology (BBPT), a relatively small battery producer in China, to develop a new lighter and faster charging lithium battery. The research and development has been done in a small factory near Beijing, with staff supplied equally from GBTS and BBPT. The new battery is now ready for production, and could be produced in either China or the UK, or both, for sale worldwide. Marketing plans and production facilities are under discussion.
You have also recently been contacted by a Russian government trade official, who has suggested that tax breaks and other incentives could be available for manufacture of electric cars in Russia, and has offered to broker talks with a Russian car manufacturer which might be interested in developing this market. You could either enter into a supplier agreement with the Russian manufacturer, or a joint venture to manufacture batteries actually in Russia, in which case bigger incentives could be available.
2: Microbial Ecology & Molecular Evolution
1) Sequence divergence is a measure of phylogenetic relatedness (i.e., biological diversity). How is this related to what people usually think of as biological diversity?
2) Other than alignment gaps, what complexities can you think of in trying to create a reasonable evolutionary model for phylogenetic analysis of entire genome sequences?
3) Standard microbiological taxonomy relies heavily of antiquated ways to distinguish or classify organisms, such as genomic %G+C and DNA:DNA hybridization. Can you imagine this changing? What are the hurdles to such a change?
4) Why do you think RFLP methods are more likely to be used to identify individuals when used for plants & animals, but to identify strains when used for microbes?
5) Different API strips, with different array of tests, are used to identify different kinds of organisms. Why do you suppose this might be necessary? Do you think you could design a more complete method, with many more tests, to identify any kind of organism? Why or why not?
6) What do you see as the relative advantages and disadvantages of each type of motility describe in Chapter 12 of Principles of Microbial Diversity to be?
7) What do you think about the hypothesis that eukaryotic flagella might be derived from spirochetes? How would you test this hypothesis? What observations would confirm or refute this hypothesis in your mind?
8) If you were interested in obtaining some novel isolates of Deinococcus or Thermus, where would you look, and how would you set up the enrichment cultures?
9) How far do you think a bacterial intracellular parasite could minimize itself? In other words, what could it do without, and what could it not do without?
10) What is the different between a minimized, obligately intracellular bacterial parasite like Chlamydia, and a virus?
11) How would you go about determining whether the paryphoplasm was similar to the periplasm of Gram-negative bacteria?
12) Members of the Plantomycetes divide by budding, and Gemmata has a double-membrane-enclosed nucleoid. Draw a picture of how you think cell division works in this organism, given that even early buds have a “nucleus”. How is your scheme similar & different from the eukaryotic cell cycle?
13) What might be the advantages or disadvantages of labeling one primer versus the other in a t-RFLP experiment? What about labeling both primers? How would you do this experiment?
14) What might you do if the restriction enzymes you use do not identify the organisms differently? In other words, what if a set of bands could be one or more of several organisms?
15) How might you deal with the fact that many of the identifications in a t-RFLP experiment are likely to be from uncultivated organisms?
16) What limitations of molecular phylogenetic analysis does DGGE or t-RFLP not improve upon?
Microbial Ecology