Overview of clinical, molecular, and therapeutic features of Niemann–Pick disease (types A, B, and C): Focus on therapeutic approaches

Authors

Kamran Hosseini, Shiraz University of Medical Sciences
Jafar Fallahi, School of Advanced Medical Sciences and Technologies
Vahid Razban, School of Advanced Medical Sciences and Technologies
Reyhaneh Zayyani Sirat, Zand Institute of Higher Education
Mahnaz Varasteh, Zand Institute of Higher Education
Vahideh Tarhriz, LSU Health Sciences Center - New OrleansFollow

Document Type

Article

Publication Date

5-7-2024

Publication Title

Cell Biochemistry and Function

Abstract

Niemann–Pick disease (NPD) is another type of metabolic disorder that is classified as lysosomal storage diseases (LSDs). The main cause of the disease is mutation in the SMPD1 (type A and B) or NPC1 or NPC2 (type C) genes, which lead to the accumulation of lipid substrates in the lysosomes of the liver, brain, spleen, lung, and bone marrow cells. This is followed by multiple cell damage, dysfunction of lysosomes, and finally dysfunction of body organs. So far, about 346, 575, and 30 mutations have been reported in SMPD1, NPC1, and NPC2 genes, respectively. Depending on the type of mutation and the clinical symptoms of the disease, the treatment will be different. The general aim of the current study is to review the clinical and molecular characteristics of patients with NPD and study various treatment methods for this disease with a focus on gene therapy approaches.

PubMed ID

38715125

Volume

42

Issue

4

Recommended Citation

Hosseini, Kamran; Fallahi, Jafar; Razban, Vahid; Sirat, Reyhaneh Zayyani; Varasteh, Mahnaz; and Tarhriz, Vahideh, "Overview of clinical, molecular, and therapeutic features of Niemann–Pick disease (types A, B, and C): Focus on therapeutic approaches" (2024). School of Medicine Faculty Publications. 2549.
https://digitalscholar.lsuhsc.edu/som_facpubs/2549
10.1002/cbf.4028