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出典(authority):フリー百科事典『ウィキペディア（Wikipedia）』「2012/10/22 16:28:40」(JST)

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Micrograph showing lipofuscin in a liver biopsy with ground glass hepatocytes; H&E stain

Lipofuscin is the name given to finely granular yellow-brown pigment granules^[1] composed of lipid-containing residues of lysosomal digestion. It is considered one of the aging or "wear-and-tear" pigments, found in the liver, kidney, heart muscle, adrenals, nerve cells, and ganglion cells. It is specifically arranged around the nucleus, and is a type of lipochrome.

Formation and turnover

It appears to be the product of the oxidation of unsaturated fatty acids, and may be symptomatic of membrane damage, or damage to mitochondria and lysosomes. Aside from a large lipid content, lipofuscin is known to contain sugars and metals, including mercury, aluminum, iron, copper and zinc.^[2]

The accumulation of lipofuscin-like material may be the result of an imbalance between formation and disposal mechanisms: Such accumulation can be induced in rats by administering a protease inhibitor (leupeptin); after a period of three months, the levels of the lipofuscin-like material return to normal, indicating the action of a significant disposal mechanism.^[3] However, this result is controversial, as it is questionable if the leupeptin-induced material is true lipofuscin.^[4]^[5] There exists evidence that "true lipofuscin" is not degradable in vitro;^[6]^[7]^[8] whether this holds in vivo over longer time periods is not clear.

Relation to diseases

Lipofuscin accumulation is a major risk factor implicated in macular degeneration, a degenerative disease of the eye.^[9]

Abnormal accumulation of lipofuscin is associated with a group of diseases of neurodegenerative disorder type called lipofuscinoses, e.g., neuronal ceroid lipofuscinosis, also known as Batten disease, as well as some other names.

Pathological accumulation of lipofuscin is implicated in Alzheimer's disease, Parkinson's disease, amyotrophic lateral sclerosis, certain lysosomal diseases, acromegaly, denervation atrophy, lipid myopathy, chronic obstructive pulmonary disease,^[10] and centronuclear myopathy. Accumulation of lipofuscin in the colon is the cause of the condition melanosis coli.

Possible therapies

Calorie restriction,^[2] vitamin E,^[2] and increased glutathione appear to reduce or halt the production of lipofuscin.

The nootropic drug piracetam appears to significantly reduce accumulation of lipofuscin in the brain tissue of rats.^[11]

Other possible treatments:

Centrophenoxine^[12]
Acetyl-L-Carnitine ^[13]
Ginko Biloba ^[14]
DMAE [1]

Wet macular degeneration can be treated using Selective Photothermolysis where a pulsed unfocused laser prodominantly heats and kills pigment- (i.e.: lipofuscin-) rich cells, leaving untouched healthy cells to multiply and fill in the gaps.^{[citation needed]} The technique is also used as a skin treatment to remove tattoos, liverspots, and in general make skin appear younger. This ability to selectively target lipofuscin has opened up research opportunities in the field of Anti-aging medicine.

Other uses

Lipofuscin quantification is used for age determination in various crustaceans such as lobsters and spiny lobsters.^[15]^[16] Since these animals lack bony parts, they cannot be aged in the same way as bony fish, in which annual increments in the ear-bones or otoliths are commonly used. Age determination of fish and shellfish is a fundamental step in generating basic biological data such as growth curves, and is needed for many stock assessment methods. Several studies have indicated that quantifying the amount of lipofuscin present in the eye-stalks of various crustaceans can give an index of their age. This method has not yet been widely applied in fisheries management mainly due to problems in relating lipofuscin levels in wild-caught animals with accumulation curves derived from aquarium-reared animals.

Notes

^ "lipofuscin" at Dorland's Medical Dictionary
^ ^a ^b ^c Chris Gaugler, "Lipofuscin", Stanislaus Journal of Biochemical Reviews May 1997
^ ML Katz, LM Rice and CL Gao, "Reversible accumulation of lipofuscin-like inclusions in the retinal pigment epithelium", Investigative Ophthalmology & Visual Science, Vol 40,(1999) pp.175-181.
^ Alexei Terman and Ulf T. Brunk, "Is Lipofuscin Eliminated from Cells?", Investigative Ophthalmology and Visual Science, (1999) vol. 40 pp.2463-2464.
^ Sallyanne Davies and Steven Ellis, "Lipofuscin Turnover", Investigative Ophthalmology and Visual Science. (1999)40 pp.1887-1888
^ Terman, A, Brunk, UT (1998). "On the degradability and exocytosis of ceroid/lipofuscin in cultured rat cardiac myocytes". Mech Ageing Dev 100 (2): 145–156. doi:10.1016/S0047-6374(97)00129-2. PMID 9541135.
^ Terman, A, Brunk, UT (1998) "Ceroid/lipofuscin formation in cultured human fibroblasts: the role of oxidative stress and lysosomal proteolysis", Mech Ageing Dev 104, pp.277-291, PMID 9818731
^ Elleder, M, Drahota, Z, Lisá V, Mares V, Mandys V, Müller J, Palmer DN.(1995) "Tissue culture loading test with storage granules from animal models of neuronal ceroid-lipofuscinosis (Batten disease): testing their lysosomal degradability by normal and Batten cells" Am J Med Genet 57, pp.213-221, PMID 7668332
^ John Lacey, "Harvard Medical signs agreement with Merck to develop potential therapy for macular degeneration", 23-May-2006
^ Joakim Allaire, François Maltais, Pierre LeBlanc, Pierre-Michel Simard, François Whittom, Jean-François Doyon, Clermont Simard & Jean Jobin (2002). "Lipofuscin accumulation in the vastus lateralis muscle in patients with chronic obstructive pulmonary disease". Muscle and Nerve 25 (3): 383–389. doi:10.1002/mus.10039.
^ Paula-Barbosa, M. et al., "The effects of Piracetam on lipofuscin of the rat cerebellar and hippocampa; neurons after long-term alcohol treatment and withdrawal", Alcoholism: Clinical and Experimental Research 15, (1991) pp. 834-838.
^ Roy D, Pathak DN, Singh R., "Effect of centrophenoxine on the antioxidative enzymes in various regions of the aging rat brain.", Exp Gerontol. 1983;18(3):185-97.
^ Amenta F, Ferrante F, et al., "Reduced lipofuscin accumulation in senescent rat brain by long-term acetyl-L-carnitine treatment.", Arch Gerontol Geriatr. 1989 Sep-Oct;9(2):147-53.
^ Huang SZ, Luo YJ, Wang L, Cai KY., "Effect of ginkgo biloba extract on livers in aged rats. ", World J Gastroenterol. 2005 Jan 7;11(1):132-5.
^ Ingebrigt Uglem, Mark Belchier & Terje Svåsand (2005). "Age determination of European lobsters (Homarus gammarus L.) by histological quantification of lipofuscin". Journal of Crustacean Biology 25 (1): 95–99. JSTOR 1549930.
^ Kerry E. Maxwell, Thomas R. Matthews, Matt R. J. Sheehy, Rodney D. Bertelsen & Charles D. Derby (2007). "Neurolipofuscin is a measure of age in Panulirus argus, the Caribbean spiny lobster, in Florida". The Biological Bulletin 213 (1): 55–66. JSTOR 25066618. http://www.biolbull.org/content/213/1/55.full.

External links for general reviews

Terman A, Brunk U (2004). "Lipofuscin". Int J Biochem Cell Biol 36 (8): 1400–4. doi:10.1016/j.biocel.2003.08.009. PMID 15147719.
Histology at neuro.wustl.edu
BU Histology Learning System: 20301loa
Destroying Lipofuscin and Destroying Cancer, FightAging.org
Unfocused Pulsed Lasers Selectively Destroy Lipofuscin, AcceleratingFuture.com

UpToDate Contents

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1. 正常な加齢 normal aging
2. アルコール性心筋症 alcoholic cardiomyopathy
3. シェーグレン・ラルソン症候群 sjogren larsson syndrome
4. 原発性色素沈着性結節性副腎皮質病変によるクッシング症候群 cushings syndrome due to primary pigmented nodular adrenocortical disease
5. 肝生検標本の解釈 interpretation of liver biopsy specimens

English Journal

Longevity of human islet α- and β-cells.

Cnop M, Igoillo-Esteve M, Hughes SJ, Walker JN, Cnop I, Clark A.SourceLaboratory of Experimental Medicine, Universite Libre de Bruxelles (ULB), Brussels, Belgium Division of Endocrinology, Erasmus Hospital, Brussels, Belgium Oxford Centre for Diabetes, Endocrinology and Metabolism, Churchill Hospital, Oxford, UK National Institutes of Health, Oxford Biomedical Research Centre, Oxford Radcliffe Hospitals Trust, Oxford, UK. Department of Mathematics, Vrije Universiteit Brussel, Brussels, Belgium.
Diabetes, obesity & metabolism.Diabetes Obes Metab.2011 Oct;13 Suppl 1:39-46. doi: 10.1111/j.1463-1326.2011.01443.x.
Pancreatic islet cell regeneration is considered to be important in the onset and progression of diabetes and as a potential cell therapy. Current hypotheses, largely based on rodent studies, indicate continuous turnover and plasticity of α- and β-cells in adults; cell populations in rodents respo
PMID 21824255

α1-adrenergic drugs modulate differentiation and cell death of human erythroleukemia cells through non adrenergic mechanism.

Fuchs R, Schraml E, Leitinger G, Stelzer I, Allard N, Haas HS, Schauenstein K, Sadjak A.SourceInstitute of Pathophysiology and Immunology, Center of Molecular Medicine, Medical University of Graz, Heinrichstrasse 31A, 8010 Graz, Austria.
Experimental cell research.Exp Cell Res.2011 Oct 1;317(16):2239-51. Epub 2011 Jul 14.
Preliminary data showed that α1-adrenergic antagonists induce apoptosis and a switch towards megakaryocytic differentiation in human erythroleukemia cells. To test the hypothesis whether survival and differentiation of erythroleukemia cells are under control of α1-adrenergic signalling, we examine
PMID 21781962

Japanese Journal

リポフスチンと黄斑色素(ルテイン,ゼアキサンチン)

尾花明
眼科 52(11), 1689-1698, 2010-10
NAID 40017352044

症例報告嚢腫壁のリポフスチンにより,黒色調を呈した外陰部アポクリン嚢胞腺腫

西山有希子,林伸和,石黒直子 [他]
臨床皮膚科 64(3), 244-246, 2010-03
NAID 40017017671

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★リンクテーブル★

リンク元	「病理学」「リポフスチン」「脂褐素」
拡張検索	「late infantile neuronal ceroid lipofuscinosis」「neuronal ceroid lipofuscinosis」