Elevated Basal Serum Tryptase: Disease Distribution and Variability in a Regional Health System

类胰蛋白酶 医学 内科学 胃肠病学 基因分型 全身性肥大细胞增多症 嗜酸性食管炎 免疫学 疾病 基因型 生物 生物化学 基因 肥大细胞
作者
Aubri M. Waters,Hyun J Park,Andrew L. Weskamp,Allyson Mateja,Megan E. Kachur,Jonathan J. Lyons,Benjamin J. Rosen,Nathan A. Boggs
出处
期刊:The Journal of Allergy and Clinical Immunology: In Practice [Elsevier BV]
卷期号:10 (9): 2424-2435.e5 被引量:35
标识
DOI:10.1016/j.jaip.2021.12.031
摘要

Background

Hereditary-alpha tryptasemia (HαT) is the most common etiology for elevated basal serum tryptase (BST). However, the utility of tryptase genotyping of individuals with elevated BST in general clinical practice remains undefined. Moreover, studies showing associations between elevated BST and chronic kidney disease (CKD), myelodysplastic syndrome (MDS), rheumatoid arthritis, or eosinophilic esophagitis did not include tryptase genotyping.

Objective

To determine the utility of tryptase genotyping among individuals with moderate elevations in BST at a regional health system.

Methods

Clinical and laboratory data from 109 subjects with basal tryptase values of 7.5 ng/mL or greater who were tested for HαT or had a disorder previously linked to elevated BST were collected retrospectively by chart review.

Results

Fifty-eight subjects had elevated BST defined as 11.5 ng/mL or greater. HαT was found in 63.8% (n = 37), 12.1% (n = 7) had CKD, and 20.7% (n = 12) had clonal myeloid disorders. A total of 6.9% (n = 4) with elevated BST had negative testing for HαT, CKD, and myeloid neoplasms. Two subjects with CKD, 1 subject with MDS, and 1 with myeloid hypereosinophilic syndrome had negative testing for HαT. Among subjects with elevated BST and more than 1 tryptase measurement, 41.5% (n = 22) had BST variability that exceeded the 20% plus 2 formula. Increased BST variability was found in subjects with HαT, all forms of mastocytosis, CKD, MDS, and those with no associated diagnosis.

Conclusions

HαT, CKD, and clonal myeloid disorders or a combination of the 3 constitute approximately 90% of individuals with elevated BST in clinical practice. Myeloid neoplasms were over-represented in this cohort relative to population prevalence data suggesting tryptase measurement selection bias by clinicians or higher prevalence. Elevated BST is associated with increased tryptase variability, regardless of etiology.
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