Cell membranes endocytosis

In addition to binding to sialic acid residues of the carbohydrate side chains of cellular proteins that the virus exploits as receptors, hemagglutinin has a second function in the infection of host cells. Viruses, bound to the plasma membrane via their membrane receptors, are taken into the cells by endocytosis. Proton pumps in the membrane of endocytic vesicles that now contain the bound viruses cause an accumulation of protons and a consequent lowering of the pH inside the vesicles. The acidic pH (below pH 6) allows hemagglutinin to fulfill its second role, namely, to act as a membrane fusogen by inducing the fusion of the viral envelope membrane with the membrane of the endosome. This expels the viral RNA into the cytoplasm, where it can begin to replicate. 

LDL (apo B-lOO, E) receptors occur on the cell surface in pits that are coated on the cytosolic side of the cell membrane with a protein called clathrin. The glycoprotein receptor spans the membrane, the B-lOO binding region being at the exposed amino terminal end. After binding, LDL is taken up intact by endocytosis. The apoprotein and cholesteryl ester are then hydrolyzed in the lysosomes, and cholesterol is translocated into the cell. The receptors are recycled to the cell surface. This influx of cholesterol inhibits in a coordinated manner HMG-CoA synthase, HMG-CoA reductase, and, therefore, cholesterol synthesis stimulates ACAT activ-... 

The calcium phosphate method was first used in 1973 to introduce adenovirus DNA into mammalian cells [3]. DNA-Calcium-phosphate complexes are formed by mixing DNA in a phosphate buffer with calcium chloride. These complexes adhere to the cell membrane and enter the cytoplasm by endocytosis. Disadvantages of DEAE-dextran and calcium phosphate transfection are a certain level of cytotoxicity, a complicated transfection procedure, and the fact that not all cell types can be transfected using these methods. 

Figure 1 General pathways through which molecules can actively or passively cross a monolayer of cells. (A) Endocytosis of solutes and fusion of the membrane vesicle with the opposite plasma membrane in an active process called transcytosis. (B) Similar to A, but the solute associates with the membrane via specific (e.g., receptor) or nonspecific (e.g., charge) interactions. (C) Passive diffusion between the cells through the paracellular space. (C, C") Passive diffusion (C ) through the cell membranes and cytoplasm or (C") via partitioning into and lateral diffusion within the cell membrane. (D) Active or carrier-mediated transport of an otherwise poorly membrane permeable solute into and/or out of a cellular barrier.

Figure 13.9 represents the TEM image of LDH particles and their cellular internalization. As expected, LDH particles are internalized by endocytosis. Figure 13.9(A) shows the cellular uptake process of LDHs after 3h of treatment, and demonstrates a successive entry of LDH by endocytosis first the LDH particles were located around the cell membrane due to their positive charge ( ), then they migrate to the membrane ruffles which are considered as endocytic bodies ( ), finally the coated intracellular vesicles were formed as early endosomes ( ). Figure 13.9(B)...

Fig. 18. (a) Representation of the tumor hypoxic state (diagram adapted from Ref. (83a). Arrow direction indicates decrease in pC>2 (< 1 mmHg), achieved for tumor depths larger than 100 pm (b) proposed mechanism for redox-mediated retention of [Cu(ATSM)] in hypoxic cells (101-105). Note Contrary to common belief cell membrane crossing solely by direct diffusion is unlikely for compounds of this family is unlikely, as indicated by fluorescence imaging work on aromatic Zn(II) analogs (vide infra). Endocytosis is the more likely uptake mechanism (112-113). 

Figure 14.10 Overview of cellular entry of (non-viral) gene delivery systems, with subsequent plasmid relocation to the nucleus. The delivery systems (e.g. lipoplexes and polyplexes) initially enter the cell via endocytosis (the invagination of a small section of plasma membrane to form small membrane-bound vesicles termed endosomes). Endosomes subsequently fuse with golgi-derived vesicles, forming lysosomes. Golgi-derived hydrolytic lysosomal enzymes then degrade the lysosomal contents. A proportion of the plasmid DNA must escape lysosomal destruction via entry into the cytoplasm. Some plasmids subsequently enter the nucleus. Refer to text for further details...

When neutrophils encounter bacteria, possibly coated with opsonin proteins of the complement system, the invaders are engulfed by the phagocytes and taken into the cells by endocytosis. A small part of the neutrophil membrane is used to create a phagosome - that is, a vacuole enclosing the bacterial cells. Within a matter of a few... 

Caveolae-dependent endocytosis occurs in cholesterol- and sphingomyelin-rich flask-shaped invaginations of the cell membrane known as caveolae (67). The shape is determined by a framework constructed by the protein caveolin. The protein binds plasma cholesterol, inserting into... 

Fittipaldi A, Ferrari A, Zoppe M, et al. Cell membrane lipid rafts mediate caveolar endocytosis of HIV-1 Tat fusion proteins. J Biol Chem 2003 278(36) 34141-34149. 

Incubation at 4°C (see section Energy Dependence on Liposome Uptake and Fusion with Cell Membranes ) and a block of metabolic activity (see section Metabolic Activity ) might also be used to block endocytosis and to detect cellular association or fusion. 

Although both LDL and HDL are primarily cholesterol particles, most of the cholesterol measured in the blood is assodated with LDL. The normal role of LDL is to deliver cholesterol to tissues for biosynthesis. When a cell is repairing membrane or dividing, the cholesterol is required for membrane synthesis. Bile acids and salts are made from cholesterol in the liver, and many other tissues require some cholesterol for steroid synthesis. As shown in Figure 1-15-6, about 80% of LDL are picked up by hepatocytes, the remainder by peripheral tissues. ApoB-100 is the only apoprotein on LDL, and endocytosis of LDL is mediated by apoB-100 receptors (LDL receptors) clustered in areas of cell membranes lined with the protdn clathrin. 

LDL particle binds with receptor In cell membrane and undergoes endocytosis... 

Another example is uptake of the iron-containing protein, transferrin, which circulates in the blood. It binds to its receptor to form a complex that enters the cell via endocytosis. The iron is then released from the endosome for use in the cell (e.g. haemoglobin formation for erythrocyte production or cytochrome production in proliferating cells). The number of transferrin receptors in the plasma membrane increases in proliferating cells and the number in the liver is increased by cytokines during infection. This results in a lower concentration of iron in the blood which decreases the proliferation of invading pathogens (Chapters 15 and 18). 

A process similar to endocytosis occurs in the reverse direction when it is known as exocytosis (Figure 5.11). Membrane-bound vesicles in the cytosol fuse with the plasma membrane and release their contents to the outside of the cell. Both endocytosis and exocytosis are manifestations of the widespread phenomenon of vesicular transport, which not only ferries materials in and out of cells but also between organelles, e.g. from the endoplasmic reticulum to the Golgi and then to the lysosomes or to the plasma membrane for secretion (Chapter 1). Many hormones are also secreted in this way, as are neurotransmitters from one nerve into a synaptic junction that joins two nerves (Chapters 12 and 14). 

In contrast, myosin I, which is not present in muscle, possesses only one head region and a short tail. Its role in cells may be involved in movement associated with membranes (endocytosis, phagocytosis). 

The protein that transports iron around the body in blood and lymph, and indeed within the cell, is transferrin (500 kDa). It has two binding sites for iron (Fe " ) when no iron is bound, it is known as apotransferrin. Transferrin picks up not only the iron absorbed from the intestine but also that released from the macrophages and then transports it to the cells that require it, which is primarily the cells in the bone marrow but also other cells that are proliferating. For uptake into the cells, the transferrin binds to a receptor on the plasma membrane and then the complex enters the cell by endocytosis. The iron is released from the complex in the cytosol where it is bound by the intra-... 

---