Glycogen Storage Disease in Adults

Overview

Journal Ann Intern Med

Specialty General Medicine

Date 1994 Feb 1

PMID 8273986

Citations 59

Authors

G M Talente

R A Coleman

C Alter

L Baker

B I Brown

R A Cannon

Y T Chen

J F CRIGLER Jr

P Ferreira

J C Haworth

G E Herman

R M Issenman

J P Keating

R Linde

T F Roe

B Senior

J I Wolfsdorf

Affiliations

Soon will be listed here.

Abstract

Objective: To identify complications amenable to prevention in adults with glycogen storage disease (GSD) types Ia, Ib, and III and to determine the effect of the disease on social factors.

Design: Case series and clinical review.

Setting: Referral medical centers in the United States and Canada.

Patients: All patients with GSD-Ia (37 patients), GSD-Ib (5 patients), and GSD-III (9 patients) who were 18 years of age or older.

Measurements: Ultrasound or radiographic studies identified liver adenomas, nephrocalcinosis, or kidney stones. Radiographic studies identified osteopenia. Reports of the clinical examination, serum chemistry results, and social data were obtained.

Results: For patients with GSD-Ia, problems included short stature (90%), hepatomegaly (100%), hepatic adenomas (75%), anemia (81%), proteinuria or microalbuminuria (67%), kidney calcifications (65%), osteopenia or fractures or both (27%), increased alkaline phosphatase (61%) and gamma-glutamyltransferase (93%) activities, and increased serum cholesterol (76%) and triglyceride (100%) levels. Hyperuricemia was frequent (89%). Patients with GSD-Ib had severe recurrent bacterial infections and gingivitis. In patients with GSD-III, 67% (6 of 9) had increased creatinine kinase activity. Four of these patients had myopathy and cardiomyopathy.

Conclusions: For GSD-Ia, hyperuricemia and pyelonephritis should be treated to prevent nephrocalcinosis and additional renal damage. For GSD-Ib, granulocyte-colony-stimulating factor may prevent bacterial infections. For GSD-III, more data are required to determine whether the myopathy and cardiomyopathy can be prevented. Most of the patients with GSD-I and GSD-III had 12 or more years of education and were either currently in school or employed.

Citing Articles

Glycogen Storage Disease Type Ia: A Retrospective Claims Analysis of Complications, Resource Utilization, and Cost of Care.

Kruger E, Nedzesky J, Thomas N, Dunn J, Grimm A J Health Econ Outcomes Res. 2025; 12(1):13-21.

PMID: 39790363 PMC: 11716495. DOI: 10.36469/001c.125886.

A case study of a liver transplant-treated patient with glycogen storage disease type Ia presenting with multiple inflammatory hepatic adenomas: an analysis of clinicopathologic and genetic data.

Wang A, Wu J, Yuan X, Liu J, Lu C BMC Med Genomics. 2024; 17(1):124.

PMID: 38711024 PMC: 11075316. DOI: 10.1186/s12920-024-01888-6.

Clinical spectrum, over 12-year follow-up and experience of SGLT2 inhibitors treatment on patients with glycogen storage disease type Ib: a single-center retrospective study.

Shao Y, Liang C, Su Y, Lin Y, Lu Z, Lin R Orphanet J Rare Dis. 2024; 19(1):155.

PMID: 38605407 PMC: 11010294. DOI: 10.1186/s13023-024-03137-6.

Endocrine involvement in hepatic glycogen storage diseases: pathophysiology and implications for care.

Rossi A, Simeoli C, Pivonello R, Salerno M, Rosano C, Brunetti B Rev Endocr Metab Disord. 2024; 25(4):707-725.

PMID: 38556561 PMC: 11294274. DOI: 10.1007/s11154-024-09880-2.

Glycogen storage diseases: An update.

Gumus E, Ozen H World J Gastroenterol. 2023; 29(25):3932-3963.

PMID: 37476587 PMC: 10354582. DOI: 10.3748/wjg.v29.i25.3932.