(biochemistry) Any of a group of lipid pigments found in cardiac and smooth muscle cells, in macrophages, and in parenchyma and interstitial cells; differential reactions include sudanophilia, Nile blue staining, fatty acid, glycol, and ethylene.
| Sci-Tech Dictionary: lipofuscin |
(biochemistry) Any of a group of lipid pigments found in cardiac and smooth muscle cells, in macrophages, and in parenchyma and interstitial cells; differential reactions include sudanophilia, Nile blue staining, fatty acid, glycol, and ethylene.
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| Food and Nutrition: lipofuscin |
A group of pigments that accumulate in several body tissues, particularly the myocardium, and are associated with the ageing process.
| Medical Dictionary: lip·o·fus·cin |
Brown pigment granules representing lipid-containing residues of lysosomal digestion.
| Veterinary Dictionary: lipofuscin |
Any of a class of fatty pigments formed by the solution of a pigment in fat. They take the form of golden granular deposits derived from lipid components of membranous organelles, and commonly occur with advancing age or vitamin E deficiency. Called also abnutzen pigment.
| Wikipedia: Lipofuscin |
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.
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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.
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], centronuclear myopathy.
Accumulation of lipofuscin in the colon is the cause of the condition melanosis coli.
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:
Wet macular degeneration can be treated using Selective Photothermolysis where a pulsed unfocused laser prodominantly heats and kills pigment (ie: lipofuscin) rich cells, leaving untouched healthy cells to multiply and fill in the gaps. The technique is also used as a skin treatment to remove tattoos, liverspots, and generally make skin appear younger. This ability to selectively target lipofuscin has opened up research opportunities in the field of Anti-aging medicine.
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| wear and tear pigment | |
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