Jenkins argues that historians face three limitations when studying the past.

 

Part 1: Jenkins argues that historians face three limitations when studying the past. Define and give an example of each of these three limitations.

Part 2: Explain Jenkins’ main argument in this chapter. What are the advantages of Jenkin’s interpretation of history? Are there any disadvantages?

In order to receive full credit for this discussion board post, you must paraphrase Jenkins at least twice. That is, summarize what he is saying in your own words. You must also include at least two direct quotations from the Jenkins reading. Whether you are paraphrasing or quoting, you must include an in-text MLA citation.

For example: According to Jenkins, the question “what is history” should be rephrased, “who is history for” (Jenkins 9).

 

 

Sample Solution

Historical research is a process of collecting and interpreting data about past events or ideas in order to find how they affected the present events and ideas. It studies possible reasons behind certain events to explain their influence on the events that followed. Historical research may not just help to figure out connections between past and present events, it can also provide the researchers with information regarding possible future events. Jenkins argues that historians face three limitations when studying the past. The major challenges to historical research revolve around the problems of sources, knowledge, objectivity, and the peculiar problems of contemporary history. Sources The problem of sources is a serious challenge to the historian in the task of reconstructing the past.

NAc receive dopamine (DA) projections from the ventral tegmental area (VTA) (Björklund and Dunnett, 2007, Ikemoto, 2007, Morales and Margolis, 2017) and this pathway play a major role in motivated behaviours, reinforcement learning and reward processing (Hamid et al., 2016; Salamone and Correa, 2012; Schultz, 2016; Watabe-Uchida et al., 2017). Like any other process, there are negative feedback pathways to balance the projections and prevent overexpression of DA. This arise from various structures (Matsui et al., 2014) but recent studies show that NAc is the main source of this inhibitory input (GABAergic input) (Beier et al., 2015; Watabe-Uchida et al., 2012). There were few conflicting results on this with studies suggesting inputs from NAc to VTA to be disinhibiting (Bocklisch et al., 2013; Chuhma et al., 2011; Xia et al., 2011) and a recent study addressing that NAc synapse onto VTA GABA as well as DA neurons via GABA-A receptor (GABAAR) and GABA-B receptor (GABABR) respectively (Edward et al., 2017). This, however, also projects a different result compared to the study done by Paladini in 1999 where inhibitory responses from the striatum to DA neurons were blocked by GABA-A antagonist hinting at pathway mediated by GABA-A instead.

In this particular study by Hongbin et al. in 2017, the shell component of the NAc is further subdivided into medial shell (NAcMed) and lateral shell (NAcLat). D1-MSN in the NAcMed is found inhibiting NAcMed-projecting DA neurons via GABAAR while NAcLat-projecting DA neurons via GABABR. D1-MSNs in the NAcLat, on the other hand, projects onto VTA GABA to result in disinhibition of NAcL

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