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Abstract Number: 2329

Do Myocardial Inflammation and Microvascular Dysfunction in RA Lead to Adverse Changes in Left Ventricular Structure and Function over Time? A Longitudinal Analysis of Participants from Rheumatoid Arthritis: Study of the Myocardium

Rabia Iqbal1, Elizabeth Park 2, Seitetsu Lee 3, Isabelle Amigues 4, Christopher Depender 2, Afshin Zartoshti 2, Jon Giles 5, Sabahat Bokhari 6 and Joan Bathon 5, 1Division on Rheumatology, Columbia University, Philadelphia, PA, 2Division on Rheumatology, Columbia University, New York, NY, 3Division of Cardiology, Columbia University, New York, NY, 4National Jewish Health, Denver, CO, 5Division of Rheumatology, Columbia University, New York, NY, 6Division of Cardiology and Nuclear Cardiology Laboratory, Columbia University, New York, NY

Meeting: 2019 ACR/ARP Annual Meeting

Keywords: heart failure and diastolic dysfunction, myocardial inflammation, Rheumatoid arthritis (RA)

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Session Information

Date: Tuesday, November 12, 2019

Title: RA – Diagnosis, Manifestations, & Outcomes Poster III: Comorbidities

Session Type: Poster Session (Tuesday)

Session Time: 9:00AM-11:00AM

Background/Purpose: The risk of developing heart failure (HF) in RA patients as compared with non-RA subjects is significantly higher even when adjusted for traditional cardiovascular (CV) risk and presence of ischemic heart disease.  HF in RA patients is characterized by preserved ejection fraction and diastolic dysfunction.  A recent prospective study demonstrated more rapid declines in diastolic function and left ventricular mass (LVM) over time in RA patients compared with control subjects.  In RA participants in the RHYTHM (RHeumatoid arthritis: studY of THe Myocardium) study, we observed a high prevalence of subclinical myocarditis (39% with visualized uptake on 18-Fluorodeoxyglucose Positron Emission Tomography-Computed Tomography [18-FDG PET-CT]) as well as microvascular dysfunction (myocardial flow reserve reduced [MFR] in 29%).  We hypothesized that RA patients with subclinical myocarditis and/or microvascular dysfunction would have greater decline in LV structure and function over time compared to RA patients without these features.

Methods: One hundred nineteen RA patients without clinical CV disease who were enrolled in RHYTHM underwent  baseline 18-FDG PET-CT to measure myocardial FDG uptake as a measure of myocardial inflammation (assessed as standardized uptake value [SUV]), and MFR as a measure of microvascular function; in addition, 3-dimensional (3D) echocardiography was performed to assess LV structure and function.  Forty-nine patients returned for a follow-up visit at 3-6-years post-baseline and underwent repeat 3D echocardiography.  The mean changes in echo parameters were calculated and Wilcoxon sign-rank tests performed to assess statistical differences between groups.  Multivariable regression models were created to assess associations between log transformed mean SUV and global MFR with change in selected echocardiographic parameters.

Results: Although in the overall group there was no significant change in the LVM index (LVMI) over time (Table 1), both higher baseline myocardial SUV (i.e., myocarditis) and lower (less favorable) MFR were associated with a greater decline in LVMI (Figures 1 and 2).  In the overall group, although there was no decline in ejection fraction (EF) over time, a significant decline in global longitudinal strain (GLS), a more sensitive measure of systolic dysfunction than EF, was observed.  With regard to diastolic function, a decline in the E/A ratio, but not in the E/E’ ratio, was observed over time.  However, there were no statistically significant relationships in changes in systolic or diastolic function with baseline SUV or MFR.

Conclusion: These results suggest that subclinical myocardial inflammation and myocardial microvascular dysfunction may be risk factors for myocardial remodeling and decline in systolic and diastolic function in individuals with RA.  Whether these subclinical features lead to clinical HF in RA is, as yet, unknown.

Table 1. Changes in selected echocardiographic parameters after 3-6-year time period, including left ventricular mass index -LVMI- adjusted for height^2.7 or body surface area -BSA-, systolic function parameters including left ventricular ejection fraction -LVEF- and global longitudinal strain -GLS-, and diastolic function parameters including E/A and E/E’ ratios.

Graph 1. Left ventricular mass -LVM- adjusted by height^2.7 decreases significantly with increasing myocardial inflammation represented by the log transformed mean standardized uptake value -SUV- on 18-FDG-PET scan.

Graph 2. Left ventricular mass -LVM- adjusted by height^2.7 decreases significantly with lower -less favorable- myocardial flow reserve -MFR- obtained with nuclear stress studies.


Disclosure: R. Iqbal, None; E. Park, None; S. Lee, None; I. Amigues, None; C. Depender, None; A. Zartoshti, None; J. Giles, Eli Lilly & Company, 5, Pfizer Inc, 2; S. Bokhari, None; J. Bathon, None.

To cite this abstract in AMA style:

Iqbal R, Park E, Lee S, Amigues I, Depender C, Zartoshti A, Giles J, Bokhari S, Bathon J. Do Myocardial Inflammation and Microvascular Dysfunction in RA Lead to Adverse Changes in Left Ventricular Structure and Function over Time? A Longitudinal Analysis of Participants from Rheumatoid Arthritis: Study of the Myocardium [abstract]. Arthritis Rheumatol. 2019; 71 (suppl 10). https://acrabstracts.org/abstract/do-myocardial-inflammation-and-microvascular-dysfunction-in-ra-lead-to-adverse-changes-in-left-ventricular-structure-and-function-over-time-a-longitudinal-analysis-of-participants-from-rheumatoid-art/. Accessed .
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