Niemann-Pick Disease

1. Niemann-Pick Disease Maggie W. George December 5, 2005

2. The Disease • Condition involving the breakdown and use of fats and cholesterol in the body • Harmful amounts of lipids accumulate in the spleen, liver, lungs, bone marrow, and brain • Autosomal recessive pattern of inheritance (two copies of the gene must be present) • Four variants: A, B, C1, and C2 • Clinical feature include: severe liver disease, breathing difficulties, developmental delay, seizures, increased muscle tone, lack of coordination, problems feeding, and inability to move eyes vertically. • No treatment

3. Variants • Types A and B: mutated SMPD1 gene • SMPD gene carries instructions for cells to produce, sphingomyelinase, which processes lipids. • Mutations lead to deficiency of sphingomyelinase and accumulations of cholesterol and lipids. • Types C1 and C2: mutated NCP1 or NCP2 gene • NCP1 gene produces a protein involved in the movement of cholesterol and lipids within a cell. • May be a cholesterol pump, which is why its mutation leads to the buildup of lipids and cholesterol in the cell membrane. • Plays a critical role in regulation of intracellular cholesterol trafficking • NCP2 gene produces protein that binds and transports cholesterol (not fully understood).

4. NCP1 v. NCP2 Gene • 95% of patients have mutations in the NPC1 gene • Mapped at chromosome 18q11 • NPC1 encodes a 1278 amino acid glycoprotein with 13 transmembrane domains. • Remainder of patients have mutations in the NPC2 gene (or HE1 gene) • Mapped at chromosome 14q24.3 • Encodes a small soluble lysosomal protein involved in cholesterol binding. • Both genes have identical biochemical patterns suggesting that the two proteins function together in cellular transport of cholesterol, glycolipids, etc. • Work together to facilitate the intracellular transport of lipids from the lysosome to other cellular sites. • Their precise functions and relationship remain unclear and are currently the subject of intense investigation.

5. NCP1 Mutations • Over 130 mutations have been identified in NPC1 • Results in Niemann-Pick Disease Type C1 • Most found within a NPC1 specific cysteine-rich domain, suggesting that the integrity of this region is crucial for normal functioning of the protein. • Mutations include: missense mutations, small deletions that generate premature stop codons, intronic mutations predicted to alter splicing, and point mutations. Specific mutation examples: • exon 20 c.2932 C>T • c.882-28 A>G (note that patients with this mutation had fibroblasts containing small amounts of mRNA without exon 7) • point mutation in exon 20 (causing frameshift and premature stop codon) • 1553G-A transition (causing a splicing error of exon 9) • 2783A-C transversion that results in a gln928-to-pro amino acid substitution • 3263A-G transition leading to a tyr1088-to-cys amino acid substitution • 530G-A change in exon 5, resulting in a cys177-to-tyr substitution • 4-bp deletion, TTAC

6. NCP2 Mutations • Results in Niemann-Pick Disease Type C2 and frontal lobe atrophy • Single amino acid changes prevents both cholesterol binding and the restoration of normal cholesterol levels in mutant cells. Specific mutation examples: 16 mutant alleles were identified representing only 5 different mutations (all had a severe impact on the protein): • 2 nonsense mutations, glu20 to ter (E20X): associated with severe rapid disease course • Results in a frameshift in exon 2, which generates a stop codon 4 codons downstream of frameshift • Lung involvement  death from respiratory failure • Glu118 to ter substitution (E118X) • Result of a G-to-T transversion at nucleotide 352 in exon 1 of HE1 gene • 1-bp deletion (27delG) • Splice mutation (IVS2+5G-A): very difference clinical presentation • Milder phenotype • Childhood onset of neurologic symptoms but prolonged survival • Missense mutation (S67P)  resulting in reduced amts of abnormal HE1 protein. *E20X was established as the most common mutant allele (56% frequency)

7. Lack of Knowledge • Unfortunately, the NCP1 and the NCP2 gene are not fully understood, which means there is no proposed structure for either. • There is a structure for the NCP2 bovine gene, but then again there is little information about the actual mutations involved.

8. Human to Bovine Relationship

11. References • http://en.wikipedia.org/wiki/Niemann-Pick_disease • http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Search&db=books&doptcmdl=GenBookHL&term=%2310+AND+gnd%5Bbook%5D+AND+138086%5Buid%5D&rid=gnd.section.231 • http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Retrieve&list_uids=15459971 • http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Retrieve&list_uids=12401890 • http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Retrieve&list_uids=15774455 • http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=pubmed&cmd=Retrieve&dopt=AbstractPlus&list_uids=12974729&query_hl=1&itool=pubmed_docsum