Receptor-mediated endocytosis

Mechanism of clathrin-dependent endocytosis.

Receptor-mediated endocytosis (RME), also called clathrin-mediated endocytosis, is a process by which cells absorb metabolites, hormones, other proteins - and in some cases viruses - (endocytosis) by the inward budding of plasma membrane vesicles containing proteins with receptor sites specific to the molecules being absorbed.

Process

Although receptors and their ligands can be brought into the cell through a few mechanisms (e.g. caveolin), clathrin-mediated endocytosis remains the best studied. Clathrin-mediated endocytosis of many receptor types begins with ligand binding and receptor activation. The ligand and receptor (often bound to an adaptor protein) then diffuse through the plasma membrane until captured by a preformed or forming clathrin-coated pit.^[1] A mature pit will pinch off from the plasma membrane forming a clathrin-coated vesicle that then uncoats and typically fuses to an early endosome. Once fused the endocytosed cargo (receptor and/or ligand) can then be sorted to lysosomal, recycling, or other trafficking pathways.^[1]

Function

The function of receptor-mediated endocytosis is diverse. It is widely used for the specific uptake of certain substances required by the cell (examples include LDL via the LDL receptor or iron via transferrin). The role of receptor-mediated endocytosis is well recognized in the downregulation of transmembrane signal transduction but can also promote sustained signal transduction.^[2] The activated receptor becomes internalised and is transported to late endosomes and lysosomes for degradation. However, receptor-mediated endocytosis is also actively implicated in transducing signals from the cell periphery to the nucleus. This became apparent when it was found that the association and formation of specific signaling complexes is required for the effective signaling of hormones (e.g. EGF). Additionally it has been proposed that the directed transport of active signaling complexes to the nucleus might be required to enable signaling as random diffusion is too slow^[3] and mechanisms permanently downregulating incoming signals are strong enough to shut down signaling completely without additional signal-transducing mechanisms.^[4]

Experiments

Using fluorescent dyes to stain the plasma membrane, it is possible to follow the internalization of plasma membrane fragments by microscopy.

Since the process is non-specific, the ligand can be a carrier for larger molecules. If the target cell has a known specific pinocytotic receptor, drugs can be attached and will be internalized.

Characteristics

Induction within minutes of exposure to excess ligand.
The formation of these vesicles is sensitive to inhibition by wortmannin
The initiation of vesicle formation can be delayed/inhibited by temperature variations

References

1 2 Sorkin, Alexander; Puthenveedu, Manojkumar A. (2013-01-01). Yarden, Yosef; Tarcic, Gabi, eds. Clathrin-Mediated Endocytosis. Springer New York. pp. 1–31. doi:10.1007/978-1-4614-6528-7_1. ISBN 978-1-4614-6527-0.
↑ Thomsen AR, Plouffe B, Cahill TJ, Shukla AK, Tarrasch JT, Dosey AM, Kahsai AW, Strachan RT, Pani B, Mahoney JP, Huang L, Breton B, Heydenreich FM, Sunahara RK, Skiniotis G, Bouvier M, Lefkowitz RJ (2016). "GPCR-G Protein-β-Arrestin Super-Complex Mediates Sustained G Protein Signaling". Cell. doi:10.1016/j.cell.2016.07.004. PMID 27499021.
↑ Howe, Charles L. (2005). "Modeling the Signaling Endosome Hypothesis: Why a Drive to the Nucleus Is Better Than a (Random) Walk". Theor. Biol. Med. Mod. 2 (1): 43. doi:10.1186/1742-4682-2-43. PMC 1276819. PMID 16236165. 2:43.
↑ Kholodenko, Boris N. (2003). "Four-Dimensional Organisation of Protein Kinase Signaling Cascades: the Roles of Diffusion, Endocytosis and Molecular Motors". J. Exp. Biol. 206 (Pt 12): 2073–82. doi:10.1242/jeb.00298. PMID 12756289. 206, 2073-2082.

External links

CytoChemistry.net- A lecture on RME with some nice pictures

Membrane transport

Mechanisms for chemical transport through biological membranes

Passive transport

Simple diffusion (or non-mediated transport)
Facilitated diffusion
Osmosis
Channels
Carriers

Active transport

Cytosis

Endocytosis	Efferocytosis Non-specific, adsorptive pinocytosis Phagocytosis Pinocytosis Potocytosis Receptor-mediated endocytosis Transcytosis

Exocytosis	Degranulation

Membrane protein: vesicular transport proteins (TC 1F)

Synaptic vesicle

SNARE

Q-SNARE	SNAP25 SNAP29 Syntaxin STX1A STX1B STX2 STX3 STX4 STX5 STX6 STX7 STX8 STX10 STX11 STX12 STX16 STX17 STX18 STX19 Munc-18: STXBP1 STXBP2 STXBP3 STXBP4 STXBP5 STXBP6

R-SNARE	Synaptobrevin/VAMP: VAMP1 VAMP2 VAMP3

Synaptotagmin

SYT1
SYT2
SYT3
SYT4
SYT5
SYT6
SYT7
SYT8
SYT9
SYT10
SYT11
SYT12
SYT13
SYT14
SYT15
SYT16
SYT17

Other

Small GTPase: RAB3A

COPI

Coatomer
- COPA
- COPB1
- COPB2
- COPE
- COPG
- COPG2
- COPZ1
- COPZ2

Archain

Small GTPase: ARF

COPII

Vesicle formation: SEC23A

Small GTPase: SAR1A

RME/Clathrin

CLTA
CLTB
CLTC

Caveolae

Other/ungrouped

Vesicle formation

Adaptor protein complex 1:	AP1AR AP1B1 AP1G1 AP1G2 AP1M1 AP1M2 AP1S1 AP1S2 AP1S3

Adaptor protein complex 2:	AP2A1 AP2A2 AP2B1 AP2M1 AP2S1

Adaptor protein complex 3:	AP3B1 AP3B2 AP3D1 AP3M1 AP3M2 AP3S1 AP3S2

Adaptor protein complex 4:	AP4B1 AP4E1 AP4M1 AP4S1

LMAN1

LYST

BLOC-1:	DTNBP1 BLOC153

BLOC-2:	HPS3 HPS5 HPS6

BLOC-3:	HPS1 HPS4

Coats:	Retromer TIP47

Small GTPase

Dynamin
- DNM1
- DNM2
- DNM3

Other

Sorting nexins

SYNRG

See also vesicular transport protein disorders

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