Ever seen ESR 100 with a normal CRP? Or CRP 150 with ESR 15?
ESR and CRP measure different aspects of inflammation and often tell different stories.
Understanding when they disagree can prevent diagnostic errors and improve clinical decision-making.
What is the biggest ESR–CRP mismatch you’ve encountered in practice?
#Rheumatology #MedTwitter #InternalMedicine @docakx@IhabFathiSulima #MedicalEducation #ClinicalPearls #FOAMed #ESR #CRP #Inflammation #RheumatologyPearls
Normal CRP ≠ No Inflammation.
Active disease may occur with a normal CRP in:
🔹 SLE (especially lupus nephritis)
🔹 Sjögren disease
🔹 Inflammatory myopathies
🔹 Systemic sclerosis
🔹 Some ANCA-associated vasculitis
Also remember:
💊 IL-6 inhibitors, steroids & JAK inhibitors can suppress CRP
🦠 Early/localized infections may have a normal CRP
Treat the patient, not the number.
#Rheumatology #CRP #Lupus #Vasculitis #Myositis @docakx@IhabFathiSulima #MedTwitter #FOAMed
📢 Explore the May 2026 issue of @BrJHaem: https://t.co/pHUW9IU345
✨ Congratulations to authors Ashleigh P. Scott and colleagues for their cover figure featured from their article: https://t.co/lnBw4YMoai
@DrAEvens | @WileyHealth
How experts treat Peripheral T- and NK-cell lymphomas
Prof Francesco D’Amore and Prof Massimo Federico break down the latest ESMO–EHA guideline for peripheral T‑ and natural killer‑cell lymphomas, highlighting the importance of accurate diagnosis in these rare, biologically diverse and often aggressive diseases. Essential listening for clinicians treating PTCLs.
🎧 Listen to the podcast: https://t.co/NDZBnBgpKN
🗃️ Access the guideline: https://t.co/BwKbBWfkr5
✨️ BJHaem Editor's pick - March ✨️
Assessment of measurable residual disease in ovarian tissue collected for fertility preservation in patients in remission from acute myeloid leukaemia: A pilot study
https://t.co/vYNR7y7rKa
@DrAEvens | @WileyHealth
🩸#MorphologyMonday | Case MM251110: May Hegglin anomaly
https://t.co/uiW9ndzY8b
✅ 28-year-old patient
✅ Mild symptoms only: occasional easy bruising, no major bleeding history.
✅ Platelets 62 × 10⁹/L
✅ Blood film: Large platelets + pale blue Dӧhle body like inclusions in neutrophils.
Diagnosis: May Hegglin anomaly
#OnlyCells #BloodFilm #Platelets #Genetics #LabDiagnostics
One of the main goals of our review article in @NEJM on MGUS was to provide clear clarifications on the concept of “monoclonal gammopathy of clinical significance” (MGCS). It’s all very confusing in the literature and can cause problems for patients if we are not totally clear of the concepts.
Read on to be 100% sure of the concepts so you can take care of your patients correctly!
1) First key concept: MGUS is a clinically indolent condition that usually remains quiet for an entire lifetime. The problem with MGUS is that it can progress to symptomatic malignancy (like multiple myeloma), or cause a variety of non-malignant, serious, and clinically important diseases that are collectively referred to as “monoclonal gammopathy of clinical significance” (MGCS).
2) Second key concept: MGCS is like the title of chapter in a textbook. It is NOT the name of a disease. Within the term “MGCS” are several distinct diseases, each of which has its own diagnostic criteria, clinical manifestations, and treatment strategies. So you simply cannot diagnose “MGCS” and treat but need to identify the specific disease. All that the term MGCS does is to alert you that MGUS can cause serious non-malignant diseases besides progression to malignancy.
3) Third key concept is: Some of the MGCS conditions are multi-system disorders like light chain amyloidosis and light chain deposition disease. Some MGCS disorders on the other hand are restricted to one organ leading to more confusing terms like “monoclonal gammopathy of renal significance” (MGRS), “monoclonal gammopathy of dermatologic significance” (MGDS), monoclonal gammopathy of neurological significance” (MGNS), and so on. These are also like titles of book chapters NOT the names of a disease. Within each term are specific unique diseases.
4) Fourth key concept is: For taking care of the patient you need to know the name of the exact disease. Not just add an umbrella term like “MGCS” or “MGRS”. So for example instead of diagnosing “MGRS” you need to be clear exactly which kidney disease the monoclonal protein is accused of causing! MGUS is so common and so many people can have a MGUS and a completely unrelated kidney disease. MGUS plus kidney disease doesn’t mean “MGRS”. Most of the time the two have nothing to do with each other.
There are specific kidney diseases that are casually related to the monoclonal protein and if we suspect MGRS for some reason we need to work up and make the specific diagnosis which needs a kidney biopsy: proliferative glomerulonephritis with immunoglobulin deposits (PGNMID), C3 glomerulonephritis, and so on. Each of these disease have their unique clinical and lab manifestations, and treatment strategies.
5) Fifth key concept is: with more and more sensitive tests for MGUS and more and more testing done for MGUS we are all going to find M proteins associated with a variety of clinical problems, 99% of which are NOT caused by the M protein. I am hugely concerned with labels like MGCS and MGRS wrongly applied. And the last thing we want is Dara-VRd for a DVT just because there is a paper that says M proteins can cause blood clots!
This Review will be a good place to start for getting all the key concepts straight. https://t.co/XErNkLVA48
Leucocytosis ...
The Handy Chart to Keep for Everyday Clinical Work
#medicine#meded#medtwitter#hematology
From My Undergraduate Teaching Slide Set
Learning Lesson : Not every WCC is Malignant :)