BUS401 Session Long Project 3

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In Modules 1 and 2 you looked at the cultural, legal, and political situation in your chosen country of Japan. Continue to do research on Japan, but now do some research on the currency and banking situation in this country.

We normally think of currency and banking risks as being something confined to third world or developing countries. But events in the past few years such as the Euro crisis or the financial crisis in the United States have shown that not even wealthy, developed countries are without risks on the financial side. So it is important for any company doing business in your country to carefully consider the risks that they face.

After you’ve done some research about financial issues in Japan, write a 2- to 3-page paper covering the following issues:

  1. The currency of your country: Is it stable? Does your country have fixed or floating exchange rates? Does the exchange rate fluctuate a lot?
  2. The banking system in your country: How safe is this system? Any recent banking crisis in your country?
  3. Overall, does the financial system in your country make it easy or difficult to do business? What kind of steps would you recommend for a company doing business in your country to hedge or minimize its financial risks? Refer to at least one of the required readings from the background materials in your answer.

Unit 7 Discussion Marketing

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Respond to your Discussion topic after you have completed your Reading and Learning Activity.

Discussion Topic: Product Strategy

What is your favorite brand of sandwich cookie? If you are like most Americans, chances are it is Oreo. In fact, Oreos are so popular that many people think Oreo was the original sandwich cookie. But they are wrong. Sunshine first marketed its Hydrox sandwich cookie in 1908. Hydrox thrived until 1912, when Nabisco (now part of Kraft) launched Oreo. With Nabisco’s superior distribution and advertising, Hydrox was soon outmatched. By 1998, Hydrox sales totaled $16 million, while Oreo’s revenues were at $374 million. Hydrox has been purchased by Keebler (subsequently purchased by Kellogg), whose elves are trying to give the cookie a major facelift. You are part of the Keebler team deciding what to do with the Hydrox brand.

Activities

  1. Can you re-create Hydrox through a name change? What kind of brand name could compete with Oreo? (Most people unfamiliar with Hydrox think it is a cleaning product.) Develop five (5) possibilities for a new name. Pick the best out of five and give your reasoning.
  2. How can you package your renewed sandwich cookie to make it more attractive on the shelf than Oreo? What about package size? Draft a brief packaging plan for the new Hydrox (or whatever name you chose).
  3. Can you modify the original formula to make something new and more competitive? Will a brand extension work here? Why or why not?

Directions for the Discussion

To obtain full credit for this assignment, you must answer thea available question as thoroughly as possible. Your answer should be thoughtful and composed using complete sentences. Please follow the Discussion Board guidelines as provided in your Syllabus.

Be sure to comment on at least two of your classmates’ posts. Your comments should be substantial and well-reasoned. Just agreeing with comments of another student does not fulfill this requirement.

Reference

Lamb, C. W., Hair, J. F., & McDaniel, C. (2014). MKTG7. Mason, OH: Cengage.

Summary of Chapter 8 and 9 and I need 5-8 pages

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Instructions listed below:

What did you learn (key chapter highlights/concepts)? Summarize the main themes within each assigned chapter and integrate these themes within this annotation report. The first section should simply identify the main themes. The second section should Integrate the main themes among the chapters. What do they have in common (tip: read the chapter objectives as a beginning framework)? Do you see any connections with previous chapter readings? Explain. What is your takeaway? The final section should take what you learned from the readings and make direct connections with the videos and instructor notes. Are there clear connections? What are they? The final section is a conclusion. Summarize your report and offer a final statement that explains how you see yourself applying these new insights within the context of your learning and/or profession.

APA, 3 references, Times New Roman, 12 Font…Master level program

References need to be the book, videos and teacher notes within the blackboard portal (it is imperative that you incorporate the videos and notes in the summary).

Chapters 8 & 9

www.uiw.edu

username: mldykes

pass: Lanell78

Please use the Ebook Professional Development: What works

Criminal Procedure Discussion Board

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While on routine patrol, you notice a car with two people inside parked behind a business that has closed for the evening. You have recognized this to be a high-crime area that has had several burglaries recently. As you pull behind the car, you shine your spotlight on the vehicle and notice the passenger in the front seat leaning down between the seats. You order the individuals out of the car and place them both in handcuffs for protection. After frisking them for weapons, you approach the passenger side of the vehicle and notice a six-pack of beer on the front floorboard. As you move the carton, you find a small container of what appears to be a controlled substance. You conduct a preliminary field test, and the substance tests positive for cocaine.

400-600 words, APA format

  • Did you have probable cause to seize the cocaine? Why or why not?
  • Does the plain view doctrine apply in this case? Why or why not?
  • What responsibility, if any, does the driver have as it relates to the seized evidence? Explain.
  • In your own words, explain the concept of exigent circumstances.
  • In your own words, explain an officer’s need to obtain a search warrant to perform a search.
  • What is the controlling constitutional issue involved in this scenario, and how does it apply? Explain.

    • gender differences in why certain crimes are committed

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    Review and reflect on the course so far. Based on what you have learned so far in this course, write at least 400–600 words on the following:

    • Assuming that males are more violent than females; does that mean crime has a biological rather than a social basis (because males and females share a similar environment)? Would you classify this as an individual or a societal issue? Explain.
    • Give examples of theories of criminology that might explain gender differences in why certain crimes are committed. Select an example of two or three crimes to respond to this question.

    It has to be APA style format and least two sources

    Introduction of Film

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    The movie I picked is SNOW WHITE AND SEVEN DWARFS, explain how three cinematic techniques and/or design elements
    have helped establish a major theme in that film.

    In 800 to 1200 words

    • Describe a major theme of the movie you have selected
      using evidence from the movie itself as well as course resources and
      other scholarly sources to support your position.
    • Identify at least three techniques (cinematography,
      lighting, acting style, or direction) and/or design elements (set
      design, costuming, or hair and makeup), and explain how these techniques
      and/or design elements contribute to the establishment of the theme.
      Reference particular scenes or sequences in your explanations.
    • State your opinion regarding the mise en scène, including
    • How the elements work together.
    • How congruent the design elements are with the theme of the movie.
    • Whether or not other techniques would be as effective (Explain your reasoning).

    Note: Remember that a theme is an overarching idea that
    recurs throughout the plot of a film. It is the distilled essence of
    what the film is about, the main design which the specific scenes and
    actions lead a viewer to understand.

    Your paper should be organized around a thesis statement that
    focuses on how the elements of your chosen feature-length film both
    establish and maintain one of its major themes. Review the Week Three sample paper, which provides an example of a well-developed analysis as well as insight on composition.

    The paper must be 800 to 1200 words in length and formatted according to APA style as outlined in the Ashford Writing Center.

    You must use at least two scholarly sources other than the textbook to support your claims. Refer to the ENG225 Research Guide

    in the Ashford University Library for guidance and to locate your

    sources. Cite your sources (including the feature-length film) within

    the text of your paper and on the reference page. For information

    regarding APA, including samples and tutorials, visit the Ashford

    Writing Center.

    Social Media and Online Collaboration tools, powerpoint

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    The purpose of this assignment is to familiarize students with the multiple collaboration tools available. Students will evaluate three online collaboration tools and choose one to suit their needs. Students will create a PowerPoint® presentation to display the advantages and disadvantages of each tool, recommend one, and explain why.

    Assignment Steps

    Resources:

    • Internet search engine/browser
    • Microsoft Office 365, Office 2016: Introductory: PowerPoint® Module 1: Creating and Editing a Presentation with Pictures
    • Microsoft Office 365, Office 2016: Introductory: PowerPoint® Module 2: Enhancing a Presentation with Pictures, Shapes, and WordArt

    Research any three online collaboration tools and recommend one.

    Evaluate and include the following parameters for each tool:

    • Ease of Use
    • Reliability and Availability
    • Cost
    • Time and Resources to Implement
    • Advantages and Disadvantages

    Create a 10- to 15-slide PowerPoint® presentation supporting your recommended choice by explaining reasons for your choice based on parameters above.

    Include the following PowerPoint® features:

    • Choose a theme for the presentation
    • At least 2 examples of Smart Art
    • At least 1 example of Word Art
    • Insert at least one shape, add text to it, and then apply a shape effect
    • Insert screenshot/picture of recommended tool displaying some of its functionality

    Format your presentation consistent with APA guidelines.

    Click the Assignment Files tab to submit your assignment.

    Develop A Strategic Action Plan to Address the Identified Issue , psychology homework help

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    Below is a 2 documents along with a copied discussion regarding the first parts of this assignment. Please read and the 2 answer the below questions accordingly. Please use APA style and citations. 3 pages

    HI All,

    Based on this assessment the people that I would need to engage for my advocacy efforts is Senator Rob Portman (he fights the opioid epidemic), Lilida, Andrew, and Melissa Schore are all owners in my current work place and which I think can make a difference in changing the opioid based programs we currently run. Since my policy is to change the current comprehensive addiction act that is set in place I would first try to contact Senator Rob Portman through email and mail. I would start by telling him my ideas and see if we can work together to make some changes to this policy because the addiction community are having an adverse reaction from using opioids. I would also have a meeting with the Schores listed above to see if we can implement a new way of treating patients who come into the facility.

    The affected population is the addiction community

    The issues due to the opioid treatment

    • People are dying
    • It is a serious health risk in the long run
    • A lot of accidents such as car accidents are caused by someone under the influence of an opioid
    • Opioid treatments can also have an adverse effect on a individual because they can have withdrawal symptoms

    The desired cost of action would be to come up with a treatment that wouldn’t have a negative effect on the patient’s body or health. I feel it is important that we address those issues because I believe if we do we will start to see a positive change in the addiction community. Individuals would be able to break free from their addictions and live addiction free lives. We must ask ourselves are we providing the best treatment and the best help for this community or can we do better.

    Below are the questions

    Include in your response:

    • Who needs to be involved in action planning efforts to maximize change efforts (i.e., programs, practices, and policies)? Who is accountable and has ownership of responsibility for facilitating change?
    • What is the role of local people as agents for or champions of community change and improvement? What roles can social workers assume in the action plan you developed?

    Family care of the mental health patient/Community setting for family health nurses

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    PLEASE READ CAREFULLY AS THESE ARE TWO SEPARATE ASSIGNMENT IN ONE. MUST BE DONE ON TWO SEPARATE DOCUMENTS

    REQUIRED READING CHAP-11,16,17

    LINK TO BOOK – http://ners.unair.ac.id/materikuliah/ebooksclub.or…

    FIRST ASSIGNMENT -DISCUSSION POST

    For this discussion, discuss the benefits and barriers to incorporating the family into care of the mental health patient. You are caring for a patient who has just been diagnosed with a mental health issue. Describe benefits and barriers that may occur when incorporating the family into caring for this patient.References:

    • Initial Post: Minimum of two (2) total references: one (1) from required course materials and one (1) from peer-reviewed references. ( 1 MUST COME FROM REQUIRED READING UP TOP)

    SECOND ASSIGNMENT ( THIS IS A PAPER)

    Overview

    The family nurse provides care within many facilities in a community. This is discussed on pages 470-476 of your text. They include nurse home visiting programs, community nursing centers, public health departments, and home education, and community education. Discuss these facilities in your community as well as access to these resources. For each resource be sure to include how families in the community benefit. Also discuss three ways in which a family health nurse may be useful in community resources. Use what you’ve learned about the role of a family health nurse and what he/she may use to help in community settings.

    Objectives

    • Examine family health nurse role in various community health settings. LINK ABOVE FOR THE CHAPTERS A MINIMUM OF 2 REFERENCE MUST COME FROM THE CHAPTER READING FROM THE BOOK ABOVE

    Minimum of four (4) total references: two (2) references from required course materials and two (2) peer-reviewed references. All references must be no older than five years (unless making a specific point using a seminal piece of information) ( AT LEAST 2 MUST COME FROM REQUIRED READING must include intext-citation

    I HAVE ATTACHED THE BOOK FOR THIS POST. WILL ALSO ATTACH THE RUBRIC FOR THE SECOND ASSIGNMENT. PLEASE FOLLOW EXACT RUBRIC TO COMPLETE THE PAPER.

    PLAGIARISM WILL NOT BE ACCEPTED. WILL BE PUT IN AN ONLINE SITE TO TEST PLAGIARISM, PLEASE FOLLOW RUBRIC OR ASSIGNMENT WILL NOT BE ACCEPTED

    Re-writing only; dont change the meaning

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    Combination therapy for early melanoma patients against immune suppression pathway

    Abstract

    Cancer is currently the leading cause of death in worldwide, Surgery, platinum-based chemotherapy, molecular targeted agents and radiotherapy are the traditional treatment used. However, the prognosis of early melanoma patients, especially those in clinical stage II and III is not as effective as patients in stage I. Therefore, new sorts of treatments are needed to be exploited for these patients.

    Immunotherapy is a promising strategy for the treatment of various types of cancer. Programmed death 1 (PD-1) and its ligand PD-L1 play a key role in tumor immune escape and the formation of tumor microenvironment, closely related with tumor generation and development. Blockading the PD-1/PD-L1 pathway could reverse the tumor microenvironment and enhance the endogenous antitumor immune responses. Utilizing the PD-1 and/or PD-L1 inhibitors has shown benefits in clinical trials. An antibody that targets programmed death-1 (PD-1) pathway has been shown to be active towards various types of cancer, including melanoma, resulting in a breakthrough therapy designation granted by FDA. These events pronounce the importance of targeting the PD-1 pathway in the treatment of melanoma cancer

    Nevertheless, monoclonal antibody targeting PD-1 therapy inherently carries a number of disadvantages such as their immunogenicity (following repeated administration) and high production costs which may limit their use and broad availability to patients. For example, recently FDA approved anti pd-1 antibody keytruda is only available for patients with metastatic cancer, for it would largely increase patient survival rate and increase tumor regression while it will also trigger severe autoimmune responses. And since PD-L1 expression correlates greatly with PD-1 expression in patient profiles, administration of treatment only targeting PD-1 leaves some patients unresponsive to immunotherapy as well.

    Therefore, in this study, we propose developing a combination therapy targeting PD-1/PD-L1 pathway for early stage melanoma patients with limited side effects. The development of this project can be organized into two parts. First, we propose a new design for immune checkpoint PD-1/PDL-1 inhibitor by formulating a nanoparticle that could inhibit the immune suppression. After designing this particle, pharmacodynamics study and in vitro, in vivo functional study will be performed. Secondly, a combinational therapy with anti-PD-1 should be tested in animal model for both its synergistic effect and treatment efficacy.

    Collectively, developing a combination therapy by Introducing nanomaterial to traditional cancer immunity treatment would help to solve unwanted side effect raised by antibody blockade action, while broadening and benefiting more patients with sufficient treatment efficacy.

    Experimental Plans

    Relevant background

    Cancer as a chronic, polygene and often inflammation-provoking disease, the mechanism of its emergence and progression is very complicated. There are many factors which impacted the development of the disease, such as: environmental factors, living habits, genetic mutations, dysfunction of the immune system and so on. At present, increasing evidence has revealed that the development and progression of tumor are accompanied by the formation of special tumor immune microenvironment. Tumor cells can escape the immune surveillance and disrupt immune checkpoint of host in several methods, therefore, to avoid the elimination from the host immune system

    Drugs targeting PD-1/PD-L1 pathway has been formulated and FDA approved for marketing. For example, pembrolizumab (Keytruda, Merck & Co., Inc., Kenilworth, NJ, USA) is a potent, humanized IgG4 monoclonal antibody against programmed death 1 (PD-1) receptor that directly blocks the interaction between PD-1 and its ligands, PD-L1 and PD-L2. Pembrolizumab has demonstrated robust, durable antitumor activity. However, because of the unmanageable and severe autoimmune side effect of using this medication in patients, it is only approved for advanced or even metastatic melanoma patients. However, it has been reported in literature that, PD-L1 expression level is independent of disease stage, but also correlates greatly with the prognosis and survival of early to mid-stage patients. Therefore, developing a combination therapy for these melanoma patients targeting immune suppression pathway i.e. PD-1/PD-L1 axis is necessary

    Spherical nucleic acids (SNAs) are structures with densely packed oligonucleotides with highly oriented functionality. Compared to their free composite oligonucleotides and nanoparticles they derived of, SNA structure confers efficient and rapid cellular uptake with great ability to modulate gene expression. Moreover, previous studies have demonstrated it also have advantages in stimulating both innate (toll-like receptor-9(TLR-9)) and adaptive immunity for cancer treatment. However, given the heterogeneity of in situ cancer population and various evading mechanisms, SNAs could be used as a platform to remove the hurdle of inhibitory signal and modulating immune response against tumor.

    Significance

    Developing a combination therapy by Introducing nanomaterial to traditional cancer immunity treatment would help to solve unwanted side effect raised by antibody blockade action, while broadening and benefiting more patients with sufficient treatment efficacy.

    Innovation

    Our immune system have a number of immune mechanism which in theory can attack/destroy tumor cells with those neo antigen, which induce a immune response. One of the major player is the cytotoxic t cells. with the help of several different kinds of immune cells, they could be trained to attack and destroy tumor cells. so if everything is working appropriately, this immune response could be quite potent.

    During cancer immunity cycle, t cell has to be activated and trained to be able to target tumor cells, however, tumor cells develop evading mechanism to escape from cytotoxic t cell attacking. PD-1/PD-L1 is one of the inhibitory signal tumor microenvironment use to tur down immune response. Therefore, to boost immune therapy efficiency, it is necessary to suppress inhibitory pathway.

    With the recently FDA approved anti pd-1 antibody keytruda for metastatic melanoma, it would largely increase patient survival rate and increase tumor regression, suggesting targeting this pathway is promising even in clinical application. However, since it’s targeting pd1 on the t cell, it has its own limitation that antoimmune side effect is inevitably. And the reason for there is no available anti pdl1 antibody, it’s because limited delivery efficency to target tumor environment. Therefore, in this project we want to benefit from SNA superior structure advantage of highly uptake in tumor environment, and knockdown/interfere pdl1 expression/function to remove the escaping mechanism, and boost t cell killing to remove tumor burden

    The concept of T-cell co-stimulation has evolved over time. The two-signal model for T-cell activation was proposed by Kevin Lafferty and co-workers as a model for the activation of naive T-cells. According to this model, T-cells require two signals to become fully activated. (Lafferty and Cunningham, 1975) The first signal, which gives specificity to the immune response, is provided by the interaction of the antigenic peptide−MHC complex with the T-cell receptor (TCR). The second, antigen-independent co-stimulatory signal, is delivered to T-cells by antigen-presenting cells (APCs) to promote T-cell clonal expansion, cytokine secretion, and effector function. (Keir et al., 2008)

    Current immunotherapies have been developed based on this model to boost or train immune CD8 T-cells to kill tumors.(Radovic-Moreno et al., 2015)[Ed1] However, tumor cells have progressively developed ways to evade the immune system. One way is through inhibitory second signal pathways like CTLA4 and PD1 interactions. Both clinical and research studies have proved that blocking these pathways could lead to enhanced tumor killing effects. (Blank et al., 2004) However, given the high cellular toxicity of present transfection reagents and the low stability of antibody-based treatment, a more stable and less toxic therapeutic approach is needed.

    Previous work from our lab have demonstrated the advantages of using the spherical nucleic acid (SNA) platform as a new strategy in cancer treatment, including for diseases such as glioblastoma multiforme (GBM), retinoblastoma, and prostate cancer.(Jensen et al., 2013; Narayan et al., 2015) Promising data have also confirmed the potential of SNAs in stimulating the immune system as potent cancer vaccines. (paper in progress[Ed2] ). Therefore, developing a new SNA targeting PDL1 as a combinational agent with the current antibody treatment could be an obvious promising step[Ed3] .

    Evaluate combination treatment of nanoparticle and anti-PD-1 antibody in melanoma mouse model

    i) First and most importantly, given the mechanism of action of anti-PD-1, several studies have tried to determine whether the efficacy of these Abs correlated with PD-L1 ligand expression in the tumor. The first studies provided evidence that there was indeed a strong link between PD-L1 expression by tumor cells and the response to anti-PD-1 Ab. Topalian et al. showed that all the responses to nivolumab were observed in patients whose tumors expressed PD-L1. Likewise, in the KEYNOTE-001 trial, responses to pembrolizumab correlated with PD-L1 expression by tumor cells. A trial assessing the effect of an anti-PD-L1 (MPDL3280A) on different types of cancer found a correlation between the level of PD-L1 present in the intratumoral immune infiltrate (but not by the tumor cells themselves) and clinical response. However, other studies did not confirm this correlation. In a meta-analysis including 1475 patients treated with nivolumab, pembrolizumab or MPDL3280A, response rates were significantly higher in PD-L1-positive tumors (34% versus 19.9%).

    Pembrolizumab (Keytruda, Merck & Co., Inc., Kenilworth, NJ, USA) is a potent, humanized IgG4 monoclonal antibody against programmed death 1 (PD-1) receptor that directly blocks the interaction between PD-1 and its ligands, PD-L1 and PD-L2. Pembrolizumab has demonstrated robust, durable antitumor activity and a manageable safety profile against several advanced malignancies. Early clinical studies of pembrolizumab employed a body-weight–based dosing strategy of 2 mg/kg every 3 weeks (Q3W) to 10 mg/kg every 2 weeks (Q2W), but in more recent trials a fixed-dose regimen (fixed with respect to body weight) has been introduced.

    Given the mechanism of action of pembrolizumab, binding to PD-1 receptors on T cells, independent on direct engagement of the molecule with tumor cells, substantial differences in exposure–response and dose–response are not expected across different tumor types. Indeed, it has been found that the pharmacokinetics (PK) of pembrolizumab are similar across oncology indications. On this basis, selection of a fixed-dose regimen focused on establishing a dose that would provide comparable (central tendency and distribution) exposures as the 2 mg/kg Q3W regimen approved in the United States for melanoma and NSCLC. The fixed dose selected also aimed to maintain exposures within the existing clinical experience range that has been established for melanoma and NSCLC and which has been associated with a lack of clinically important differences in efficacy or safety

    the central tendency (mean, median) at 200 mg Q3W is modestly increased (~35%) relative to 2 mg/kg Q3W for all PK measures (AUCss, 0-6weeks, Cmax, ss and Ctrough, ss), while these values are ~25% of those obtained at 10 mg/kg Q3W. Intersubject variation (% CV) is similar for all regimens and the 10–90% percentiles are largely overlapping for 2 mg/kg and 200 mg Q3W. A minimum effective administration of anti-PD-1 antibody should be tested in mouse model we developed. The administration route, dose amount and dose schedule should be tested in vivo.

    Regarding to the in vivo biomarkers they tested for anti-PD1 mAb, A multitude of biomarkers has been studied, predominantly involving indices from the patient’s tumor (tumor cells or cells from the microenvironment) or blood (circulating cells or serum).Treatment with anti-PD-1 Ab was associated with increased circulating IFN-γ, IL-18 and ITAC (an IFN-γ inducible chemokine which is chemotactic for activated T cells) and decreased IL-6. However, no correlation was found with clinical efficacy. The presence of lymphocytes within the tumor is another favorable prognostic factor in numerous cancers treating with checkpoint inhibitor antibody. In patients with metastatic melanoma, an increase in lymphocyte infiltrate in the tumor between baseline and at 3 weeks after treatment initiation correlated with clinical response. Moreover, in melanoma patients, response rate was better in patients with high numbers of peri- and intratumoral CD8 T cells in their pretreatment samples. Analysis of biopsies after treatment showed a correlation between a high ratio of intratumoral CD8/regulatory T cells and tumor necrosis. Moreover, in patients with metastatic melanoma, Tumeh et al. found that clinical response to anti-PD1 therapy (pembrolizumab) correlated with (i) a more clonal (i.e. more restricted, less diverse) TCR repertoire in pretreatment tumor samples and (ii) an increased clonal expansion of T cells in the tumor after anti-PD1 therapy.

    ii) Synergistic effect of administrating both nanoparticle and antibody should be tested in vivo. A overall PD-L1 expression level, circulating cytokine, and tumor microenvironment remodeling should be 3 factors to be valued following combination treatment. A tumor regression curve and mouse survival rate should also be performed

    [Ed1]Not sure if I would reference this here. As written, it makes it sound like there are disadvantages to our work. I don’t think you should describe it in that way.

    [Ed2]`

    [Ed3]Add a sentence or two about fundamental scientific issues you will explore.