BGPT: Paper Review: The value of C-reactive protein in emergency medicine

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Core takeaway

This narrative review argues CRP is nonspecific for ruling in/out most ED diagnoses, but can be useful for prognosis/monitoring and sometimes supports discrimination between etiologies (e.g., some infection vs non-infection contexts), while emphasizing that imaging + clinical evaluation remain primary.

Source:

Long Explanation

Paper Review (Visual-First): “The value of C-reactive protein in emergency medicine”

Narrative review by Yu-Jang Su (Journal of Acute Disease, 20 March 2014). DOI: 10.1016/S2221-6189(14)60001-9

What the paper is trying to do

Provide a narrative review of CRP’s diagnostic (largely adjunct), prognostic, and monitoring value across common ED emergencies—while cautioning against over-reliance on single CRP values.

How the paper argues

CRP is an acute-phase reactant (inflammatory “signal”) used frequently in ED.
It is often too nonspecific to rule in/out most ED diagnoses from a single value.
CRP can help with risk/prognosis and serial monitoring in multiple conditions.
For definitive diagnosis, the paper repeatedly points to history/exam and imaging as primary.

Visual Map: Where the paper places CRP in ED workflows

The diagram summarizes the paper’s overall positioning: CRP is primarily adjunctive and monitoring/prognostic across ED emergencies, not a single-value definitive diagnostic test.

Condition-by-condition claims (what the paper says CRP is for)

The paper provides condition sections; below is a structured extraction of the type of CRP utility it claims (diagnosis vs prognosis/monitoring vs discrimination), not an assessment of effect sizes (because this review often does not provide full numerical tables in the provided text).

ED emergency	CRP role claimed	Key caution / nuance in paper
Acute coronary syndrome (ACS)	Baseline CRP as independent predictor of mortality; hsCRP discussed for prognosis; CRP linked to plaque destabilization discussion	Paper reports that routine hsCRP may not improve diagnostic accuracy in a chest pain observation unit context
Aortic dissection	Admission CRP and peak CRP associated with prognosis/long-term outcomes	Higher CRP associated with worse short- and long-term events
Appendicitis	CRP used as a reference to support disposition decision-making in acute abdominal pain; serial CRP suggested to be helpful after 12–24h	Cites that normal CRP with normal WBC makes appendicitis unlikely; also highlights obesity can impair reliability in children
Cholecystitis	Not suitable for diagnosis; predicts severity and response to therapy	Paper explicitly states CRP cannot play a suitable role in diagnosis
Gout	CRP not a reliable diagnostic test for gout	Hyperuricemia does not necessarily raise CRP; benzbromarone may affect CRP (as cited in paper)
Meningitis	Serial CRP distinguishes Gram-negative bacterial from viral meningitis (as cited)	Paper positions procalcitonin as an adjunct with higher/earlier diagnostic value than CRP in this context
Pancreatitis	CRP used for severity assessment and monitoring (e.g., warning of severe course)	Paper frames CRP as severity tool rather than making diagnosis
Pelvic inflammatory disease (PID)	CRP used for monitoring treatment response; CRP declines in responders	TOA vs no TOA differences in CRP normalization timing (as described)
Pneumonia	CRP is more for prognosis and therapy response than diagnosis	Failure of CRP to fall by 50% by day 4 associated with worse outcomes (as cited)
Sepsis (early)	Not reliable/meaningful in early postoperative setting; pseudo-elevation from tissue damage discussed	Paper argues procalcitonin is superior for neonatal/LONS contexts and likely for sepsis biomarker differentiation
Stroke	Higher hsCRP in ischemic vs hemorrhagic; CRP elevation associated with mortality risk	Paper emphasizes concurrent infections need evaluation
Urinary tract infection (UTI)	CRP not accurate for localizing site of UTI in girls without pyelonephritis signs; useful as part of evaluation localization only in some contexts (ESR/diff counts referenced)	Paper highlights that leukocytosis may be absent in febrile UTI

The table content is derived from the provided full-text sections of the paper.

Evidence-grade critique (skeptical lens)

1) Study design & synthesis mode

The article is a narrative review (no primary study methods described; no new datasets). That design choice makes the conclusions more susceptible to selection of cited studies, heterogeneous assays/cutoffs, and unequal weighting of stronger vs weaker evidence.

2) Nonspecificity is acknowledged—but interpretation risk remains

The paper repeatedly emphasizes CRP’s inability to reliably discriminate bacteremia vs nonbacteremic infection using CRP alone, and concludes that a single CRP value should not rule in/out most ED diagnoses. That is directionally consistent with later ED/biomarker syntheses that find established biomarkers often have limited standalone prognostic value for some endpoints in heterogeneous ED presentations.

3) Calibration/threshold variability problem

The review uses many cutoff statements across conditions, but narrative reviews typically cannot fully account for assay differences, timing of sampling, and population differences. That creates a reproducibility/transportability risk: a cutoff from one setting may not behave similarly elsewhere.

4) Missing: explicit risk-of-bias weighting and quantification

A narrative review generally does not provide a PRISMA-style structured search, QUADAS/DTA-style or ROB2/QUIPS-style risk-of-bias assessment per study, or pooled effect estimates. That means the reader must accept the authors’ selection and interpretation of the evidence without transparent quality weighting.

What would most likely change (or falsify) the paper’s stance?

Better discrimination: large prospective ED studies showing that a defined CRP-based rule (single value or serial pattern) improves diagnostic accuracy for specific emergencies beyond clinical assessment + imaging, with external validation.
Robust prognostic utility: evidence that CRP (alone or in predefined combinations) predicts ED-important outcomes consistently across settings and assays (reduced heterogeneity).
Demonstrated added value: decision-analytic studies proving that CRP-guided pathways improve patient-relevant outcomes or safety (or reduce harm from delayed/over-treatment), rather than only improving surrogate biomarkers.

A contemporary example of the general challenge in ED prognostic biomarkers is reflected in the sepsis evidence synthesis showing limited standalone prognostic value and large heterogeneity across studies.

Quick “how to use this review” checklist (skeptical, actionable)

Treat CRP as adjunct, not a stand-alone rule-in/out.
Prefer trend/serial changes when the review explicitly frames monitoring as useful (where the evidence cited supports it).
When applying cutoffs, verify assay/unit compatibility and timing assumptions (the paper implicitly warns against single-value decisions).
Use clinical assessment + imaging as the decisive diagnostic step for conditions where the review states CRP adds little diagnostic value.

Author reviews (Bespoke BGPT links)

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Updated: April 14, 2026