Standardized indolent systemic mastocytosis evaluations across a health care system: implications for screening accuracy

Author:

McMurray Jeremy C.1ORCID,Pacheco Curtis S.2,Schornack Brandon J.1,Sun Xiaoping3,Brunader Janet A.4,Scott Alexis E.4,Ariza Juan S.5,Kou Chung-Ting J.6,Costantino Ryan C.7,Pittman Luke M.1,Adams Karla E.8,Waters Aubri M.9,Pryor Eric M.10,Lyons Jonathan J.1112ORCID,Metcalfe Dean D.13ORCID,Maric Irina3,Boggs Nathan A.114ORCID

Affiliation:

1. 1Allergy and Immunology Service, Walter Reed National Military Medical Center, Bethesda, MD

2. 2Department of Internal Medicine, Brooke Army Medical Center, San Antonio, TX

3. 3Hematology Section, Department of Laboratory Medicine, National Institutes of Health, Bethesda, MD

4. 4Immunization Healthcare Division, Defense Health Agency, Falls Church, VA

5. 5Department of Internal Medicine, Walter Reed National Military Medical Center, Bethesda, MD

6. 6Hematology and Oncology Service, Brooke Army Medical Center, San Antonio, TX

7. 7Enterprise Intelligence and Data Solutions Program Office, Program Executive Office, Defense Healthcare Management Systems, San Antonio, TX

8. 8Department of Medicine, Allergy and Immunology Service, Wilford Hall Ambulatory Surgical Center, Lackland Air Force Base, San Antonio, TX

9. 9Allergy and Immunology Service, Brooke Army Medical Center, San Antonio, TX

10. 10Hematopathology Service, Department of Pathology, Walter Reed National Military Medical Center, Bethesda, MD

11. 11Division of Allergy and Immunology, Department of Medicine, University of California San Diego, La Jolla, CA

12. 12Veterans Affairs San Diego Health Care System, La Jolla, CA

13. 13Mast Cell Biology Section, Laboratory of Allergic Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD

14. 14Department of Medicine, Uniformed Services University, Bethesda, MD

Abstract

Abstract Timely diagnosis of systemic mastocytosis (SM) remains challenging because of care heterogeneity. We implemented a standardized approach for SM screening and diagnosis using a novel health care system–wide international screening registry. A retrospective analysis assessed rates of SM, cutaneous mastocytosis (CM), and molecular diagnoses before and 2 years after care standardization. The accuracy of individual and combined SM screening tests, basal serum tryptase (BST) ≥11.5 and ≥20.0 ng/mL, REMA ≥2, monomorphic maculopapular CM (MPCM), and elevated BST based upon tryptase genotype, was analyzed. Tryptase genotyping and high-sensitivity KIT p.D816V testing increased substantially 2 years after care standardization. SM diagnoses doubled from 47 to 94, and KIT p.D816V molecular diagnoses increased from 24 to 79. Mean BST and KIT p.D816V variant allele frequency values were significantly lower in patients diagnosed after standardization. Hereditary-alpha tryptasemia prevalence was increased in SM before care standardization (4/30 [13.3%]) but reflected the general population prevalence 2 years later at (5/76 [6.6%]). Elevated BST based upon genotype and BST ≥11.5 ng/mL had the highest sensitivities at 84.2% and 88.3%, respectively. The presence of monomorphic MPCM, elevated BST based upon tryptase genotype, and the combination of REMA ≥2 with elevated BST based upon tryptase genotype had specificities >90%. BST >20.0 ng/mL had low sensitivity and specificity and was not required to establish any indolent SM (ISM) diagnosis. Care standardization increased SM diagnosis rates, particularly in patients with low BSTs. Stratifying BST based upon genotype had the best overall sensitivity and specificity of any ISM screening test and improved the REMA score specificity.

Publisher

American Society of Hematology

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