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NRNP 6635 FINAL EXAM LATEST 2026/2027 | Psychopathology and Diagnostic Reasoning | Already Graded A | Walden University | Pass Guaranteed - A+ Graded

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Pass the NRNP 6635 Final Exam on your first attempt with this latest 2026/2027 resource for Psychopathology and Diagnostic Reasoning at Walden University, already graded A. This A+ Graded resource contains final exam questions and verified answers covering all key content areas including foundations of psychopathology, DSM-5-TR diagnostic classification, clinical interviewing techniques, mental status examination (MSE), differential diagnosis process, neurodevelopmental disorders (autism spectrum disorder, ADHD, intellectual disability), schizophrenia spectrum and psychotic disorders (schizophrenia, schizoaffective, delusional disorder, brief psychotic disorder), bipolar I and II disorders, cyclothymic disorder, depressive disorders (major depressive disorder, persistent depressive disorder, PMDD, disruptive mood dysregulation disorder), anxiety disorders (GAD, panic disorder, agoraphobia, social anxiety, specific phobias, separation anxiety), OCD and related disorders (OCD, body dysmorphic, hoarding, trichotillomania, excoriation), trauma and stressor-related disorders (PTSD, acute stress disorder, adjustment disorder, reactive attachment disorder, disinhibited social engagement disorder), dissociative disorders (DID, dissociative amnesia, depersonalization/derealization), somatic symptom disorders, factitious disorder, feeding and eating disorders (anorexia, bulimia, binge-eating, pica, rumination, ARFID), elimination disorders (enuresis, encopresis), sleep-wake disorders (insomnia, hypersomnolence, narcolepsy, sleep apnea, circadian rhythm disorder, parasomnias, restless leg syndrome), sexual dysfunctions (delayed ejaculation, erectile disorder, female orgasmic disorder, female sexual interest/arousal disorder, genito-pelvic pain/penetration disorder, male hypoactive sexual desire disorder, premature ejaculation), gender dysphoria, disruptive impulse-control and conduct disorders (oppositional defiant disorder, intermittent explosive disorder, conduct disorder, pyromania, kleptomania), substance-related and addictive disorders (alcohol, opioids, stimulants, cannabis, sedatives, hallucinogens, inhalants, gambling disorder), neurocognitive disorders (delirium, major/mild neurocognitive disorder due to Alzheimer's, vascular, Lewy body, frontotemporal, Parkinson's, HIV, prion disease, Huntington's, TBI), personality disorders (Cluster A: paranoid/schizoid/schizotypal, Cluster B: antisocial/borderline/histrionic/narcissistic, Cluster C: avoidant/dependent/OCPD), and paraphilic disorders (voyeuristic, exhibitionistic, frotteuristic, masochism, sadism, pedophilic, fetishistic, transvestic). Each answer includes clear rationales to reinforce diagnostic reasoning using DSM-5-TR criteria. Perfect for PMHNP students preparing for the NRNP 6635 final exam. With our Pass Guarantee, you can confidently prepare for your Psychopathology and Diagnostic Reasoning final exam. Download your complete NRNP 6635 Final Exam latest guide instantly!

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NRNP 6635 FINAL EXAM LATEST 2026/2027 |
Psychopathology and Diagnostic Reasoning | Already
Graded A | Walden University | Pass Guaranteed - A+ Graded



Section 1: Neurobiology, Genetics, & Psychopharmacology
Foundations (Q1-18)

Q1: A 28-year-old patient with schizophrenia is prescribed risperidone. The PMHNP
explains that risperidone's therapeutic effect primarily results from antagonism of which
dopamine pathway?

A. Mesocortical pathway—improving positive symptoms through prefrontal cortex
modulation
B. Mesolimbic pathway—reducing positive symptoms through ventral tegmental area to
nucleus accumbens blockade
C. Nigrostriatal pathway—preventing extrapyramidal symptoms through striatal
dopamine enhancement
D. Tuberoinfundibular pathway—increasing prolactin through pituitary dopamine
stimulation

Correct Answer: B
B. Mesolimbic pathway—reducing positive symptoms through ventral tegmental area to
nucleus accumbens blockade [CORRECT]
Rationale: Atypical antipsychotics like risperidone block D2 receptors in the mesolimbic
pathway, reducing hyperdopaminergic activity responsible for positive symptoms
(hallucinations, delusions). A is incorrect because mesocortical hypodopaminergia
relates to negative symptoms, not positive. C is incorrect because nigrostriatal blockade
causes EPS, not prevents it. D is incorrect because tuberoinfundibular blockade
increases prolactin (side effect), not a therapeutic mechanism.

,Q2: A PMHNP is evaluating a patient with treatment-resistant depression.
Pharmacogenomic testing reveals the patient is a CYP2D6 poor metabolizer. Which
antidepressant would require the most significant dose reduction to avoid toxicity?

A. Sertraline
B. Venlafaxine
C. Fluoxetine
D. Bupropion

Correct Answer: C
C. Fluoxetine [CORRECT]
Rationale: Fluoxetine is primarily metabolized by CYP2D6; poor metabolizers
accumulate parent drug and active metabolite norfluoxetine, increasing risk of serotonin
syndrome and QT prolongation. A (sertraline) uses multiple CYP pathways. B
(venlafaxine) is metabolized by CYP2D6 but has active metabolite with different profile.
D (bupropion) is metabolized by CYP2B6, not 2D6.

Q3: The BDNF Val66Met polymorphism has been most consistently associated with:

A. Increased risk of schizophrenia through dopamine receptor dysregulation
B. Reduced activity-dependent BDNF secretion and increased vulnerability to
stress-related depression
C. Enhanced serotonin reuptake transporter function and anxiety resilience
D. Altered GABA receptor subunit composition and panic disorder

Correct Answer: B
B. Reduced activity-dependent BDNF secretion and increased vulnerability to
stress-related depression [CORRECT]
Rationale: The Met allele impairs activity-dependent BDNF release from synaptic
vesicles, reducing neuroplasticity and increasing depression risk, particularly with
childhood adversity. A describes COMT or DISC1 associations. C describes SLC6A4
(serotonin transporter) polymorphisms. D describes GABAergic mechanisms unrelated
to BDNF.

,Q4: A patient on chronic haloperidol develops tardive dyskinesia. The PMHNP
understands this results from:

A. Up-regulation of D2 receptors in the nigrostriatal pathway due to chronic antagonism
B. Down-regulation of D2 receptors in the mesolimbic pathway causing dopamine
supersensitivity
C. Destruction of GABAergic interneurons in the striatum
D. Up-regulation of muscarinic receptors in the tuberoinfundibular pathway

Correct Answer: A
A. Up-regulation of D2 receptors in the nigrostriatal pathway due to chronic antagonism
[CORRECT]
Rationale: Chronic D2 antagonism causes compensatory up-regulation
(supersensitivity) of postsynaptic D2 receptors in the nigrostriatal pathway, leading to
tardive dyskinesia when drug is withdrawn or at end-of-dose intervals. B describes
mesolimbic changes related to psychosis relapse, not TD. C describes Huntington's
mechanism. D is incorrect—TD is dopaminergic, not cholinergic.

Q5: The SLC6A4 gene (serotonin transporter) 5-HTTLPR short allele has been
associated with:

A. Increased serotonin transporter expression and reduced depression risk
B. Decreased serotonin transporter expression and increased stress sensitivity
C. Altered dopamine D2 receptor density and impulsivity
D. Enhanced norepinephrine reuptake and anxiety resilience

Correct Answer: B
B. Decreased serotonin transporter expression and increased stress sensitivity
[CORRECT]
Rationale: The short (S) allele reduces 5-HTT expression and function, leading to less
efficient serotonin reuptake, synaptic serotonin accumulation, and increased amygdala
reactivity to stress—creating a gene × environment interaction for depression. A
describes the long (L) allele. C and D describe unrelated neurotransmitter systems.

, Q6: A PMHNP prescribes aripiprazole for a patient with bipolar disorder. The unique
pharmacodynamic profile of aripiprazole is best described as:

A. Pure D2 antagonist with high affinity for all dopamine receptors
B. D2 partial agonist with functional antagonism at hyperdopaminergic synapses and
agonism at hypodopaminergic synapses
C. Pure 5-HT2A antagonist with no dopamine receptor activity
D. D1 full agonist with D3/D4 antagonism

Correct Answer: B
B. D2 partial agonist with functional antagonism at hyperdopaminergic synapses and
agonism at hypodopaminergic synapses [CORRECT]
Rationale: Aripiprazole's partial agonism (intrinsic activity ~25%) stabilizes dopamine
transmission—antagonizing when dopamine is high (mesolimbic) and agonizing when
low (mesocortical). A describes typical antipsychotics. C describes pure 5-HT2A
antagonists (e.g., mirtazapine). D is pharmacologically incorrect.

Q7: A patient with Parkinson's disease develops visual hallucinations. The PMHNP
recognizes this most likely results from:

A. Excessive dopaminergic medication causing mesolimbic pathway hyperactivity
B. Lewy body pathology directly affecting the visual cortex
C. Anticholinergic medication toxicity
D. Progressive supranuclear palsy misdiagnosis

Correct Answer: A
A. Excessive dopaminergic medication causing mesolimbic pathway hyperactivity
[CORRECT]
Rationale: Dopaminergic medications (levodopa, dopamine agonists) can overstimulate
mesolimbic pathways, producing hallucinations and psychosis—distinguishable from
dementia with Lewy bodies hallucinations by temporal relationship to medication. B
describes DLB mechanism but not medication-induced. C causes delirium, not isolated
hallucinations. D is unrelated.

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