Molekulargenetisches Labor
Zentrum für Nephrologie und Stoffwechsel
Das Membranprotein, welches vom MCP-Gen kodiert wird, besitzt eine wichtige Funktion in der Complement-Kaskade und stellt den zellulären Rezeptor des Masernvirus. Heterozygote Mutationen können ein atypisches (hereditäres) hämolytisch urämisches Syndrom (aHUS) auslösen. Theoretisch ist auch eine Beeinflussung der Infektanfälligkeit gegenüber Masern denkbar.
Das der Membranrezeptor passiert die Basalmembran nur einmalig. Das kurze N-terminale Ende befindet sich intrazellulär. Extrazellulär unterscheiden wir vom C-terminalen Ende ausgehend 4 SCR-(short consensus repeat)-Domainen und anschließend zwei serin-, threonin- und prolin-reiche Domainen, STR.
Der Rezeptor for das Complementsystem (CD46) wird auf allen Zellen außer Erythrozyten gefunden.
Heterozygote Mutationen können entweder zu einer verminderten Anzahl von Rezeptoren auf der Zelloberfläche führen. Dies ist bei etwa 75% der Mutationen der Fall. Die übrigen Mutationen zeigen zwar eine normale oder eher erhöhte Membranexpression, aber eine verminderte Funktion. 93% der Mutationen finden sich in einer der 4 extrazellulären SCR-(short consensus repeat)-Domainen, die für die Regulation der Complementfunktion verantwortlich sind.
Die Penetranz der heterozygoten MCP-Mutationen für das atypische HUS beträgt wird mit 54% angegeben.[Error: Macro 'ref' doesn't exist]
| Klinisch | Untersuchungsmethoden | Familienuntersuchung |
| Bearbeitungszeit | 5 Tage | |
| Probentyp | genomische DNS |
| Klinisch | Untersuchungsmethoden | Hochdurchsatz-Sequenzierung |
| Bearbeitungszeit | 25 Tage | |
| Probentyp | genomische DNS |
| Klinisch | Untersuchungsmethoden | Direkte Sequenzierung der proteinkodierenden Bereiche eines Gens |
| Bearbeitungszeit | 20 Tage | |
| Probentyp | genomische DNS |
| Klinisch | Untersuchungsmethoden | Multiplex ligationsabhängige Amplifikation |
| Bearbeitungszeit | 20 Tage | |
| Probentyp | genomische DNS |
| 1. |
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OMIM.ORG article Omim 120920
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| 44. |
Orphanet article Orphanet ID 119259
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| 45. |
NCBI article NCBI 4179
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| 46. |
Wikipedia Artikel Wikipedia DE (Membrancofaktorprotein)
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