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Phagosome Formation

The process of engulfing a foreign particle - phagocytosis - is of fundamental importance for a wide diversity of organisms. From simple unicellular organisms that use phagocytosis to obtain their next meal, to complex metazoans in which phagocytic cells represent an essential branch of the immune system, cells have been equipped with a repertoire of signaling molecules that serve to bring about this complex event. Despite the diversity of cell-types and end-purposes that make use of this phenomenon, all phagocytic processes are driven by a finely controlled rearrangement of the actin cytoskeleton to form the phagosome upon activation of specific cell-surface receptors that identify the particle or cell of interest....

Phagosome Formation

Pathway Summary

The process of engulfing a foreign particle - phagocytosis - is of fundamental importance for a wide diversity of organisms. From simple unicellular organisms that use phagocytosis to obtain their next meal, to complex metazoans in which phagocytic cells represent an essential branch of the immune system, cells have been equipped with a repertoire of signaling molecules that serve to bring about this complex event. Despite the diversity of cell-types and end-purposes that make use of this phenomenon, all phagocytic processes are driven by a finely controlled rearrangement of the actin cytoskeleton to form the phagosome upon activation of specific cell-surface receptors that identify the particle or cell of interest.Multiple receptors simultaneously recognize microbes both through direct binding of microbial surface ligands and by binding to opsonins that have been deposited on the microbial surface. These include: the FcRs(Fc receptors), CRs (complement receptors), non-complement-receptor integrins, lectins and the diverse group of scavenger receptors. In the later case, recognition and binding of microbes by phagocytes is assisted by coating these cells with opsonins, such as complement and Igs (immunoglobulins), that mark them for ingestion and facilitate the process of internalization.Complement-receptor-mediated phagocytosis is morphologically distinct from that mediated by FcRs, although both processes require actin polymerization. Complement-opsonised particles sink into the phagocyte; there is minimal membrane disturbance, and internalization does not usually lead to an inflammatory response or oxidative burst. Internalization by non-complement-receptor integrins such as Alpha5Beta1 and Alpha5Beta3, lectins such as the mannose receptor, the LPS (lipopolysaccharide) receptor CD14 and the scavenger receptors appear to be morphologically dynamic, as in the case of Fc receptors. Membrane is extended around the attached particle, and there is transient membrane ruffling in surrounding areas of the cell. Two members of the scavenger receptor family: SR-A (scavenger receptor-A or macrophage scavenger receptor) and MARCO (macrophage receptor with collagenous structure) have been implicated in binding and internalizing microbes. SR-A is expressed on most macrophages and binds whole bacteria as well as the microbial cell wall components, LTA (lipoteichoic acid) and LPS. The mannose receptor (that binds mannan) and Dectin1 (CLEC7A) (that binds beta-glucan) mediate phagocytosis of yeast and zymosan. Both FN (fibronectin) and VTN (vitronectin) can non-specifically opsonize pathogens.Toll-like receptors (TLRs) are a variety of pattern recognition receptors (PRR) that recognize pathogen associated molecular patterns (PAMP) on infectious agents. Binding of the infectious agents to TLRs stimulates phagocytosis and the release of inflammatory cytokines from the phagocytes. TLRs detect a broad range of microbial products including LPS, PGN (peptidoglycan), and bacterial lipopeptides. Several TLR family members are actively recruited to phagosomes during microbe internalization where they sample the contents of the phagosomes to determine the nature of the microbes being ingested. Dozens of signaling molecules including actin binding proteins, membrane traffic regulators, ion channels, kinases, and lipases are activated during phagocytosis of microbes and may contribute to efficient internalization. Certain signaling molecules stand out both as participating in phagocytosis and as participating in many other signaling pathways. PI3K, PLC (phospholipase-C), RhoGTPases, and PKCs (protein kinase-C) are integration points for regulation of phagocytosis.

Phagosome Formation Genes list

Explore Genes related to Phagosome Formation
ABHD3
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Human
abhydrolase domain containing 3, phospholipase
ACKR1
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Human
atypical chemokine receptor 1 (Duffy blood group)
ACKR3
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Human
atypical chemokine receptor 3
ACKR4
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Human
atypical chemokine receptor 4
ACTR2
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Human
actin related protein 2
ACTR3
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Human
actin related protein 3
ADCYAP1R1
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Human
ADCYAP receptor type I
ADGRA1
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Human
adhesion G protein-coupled receptor A1
ADGRA2
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Human
adhesion G protein-coupled receptor A2
ADGRA3
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Human
adhesion G protein-coupled receptor A3
ADGRB1
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Human
adhesion G protein-coupled receptor B1
ADGRB2
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Human
adhesion G protein-coupled receptor B2
ADGRB3
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Human
adhesion G protein-coupled receptor B3
ADGRD1
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Human
adhesion G protein-coupled receptor D1
ADGRD2
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Human
adhesion G protein-coupled receptor D2
ADGRE1
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Human
adhesion G protein-coupled receptor E1
ADGRE2
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Human
adhesion G protein-coupled receptor E2
ADGRE3
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Human
adhesion G protein-coupled receptor E3
ADGRE5
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Human
adhesion G protein-coupled receptor E5
ADGRF1
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Human
adhesion G protein-coupled receptor F1
ADGRF2
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Human
adhesion G protein-coupled receptor F2
ADGRF3
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Human
adhesion G protein-coupled receptor F3
ADGRF4
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Human
adhesion G protein-coupled receptor F4
ADGRF5
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Human
adhesion G protein-coupled receptor F5
ADGRG1
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Human
adhesion G protein-coupled receptor G1
ADGRG2
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Human
adhesion G protein-coupled receptor G2
ADGRG3
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Human
adhesion G protein-coupled receptor G3
ADGRG4
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Human
adhesion G protein-coupled receptor G4
ADGRG5
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Human
adhesion G protein-coupled receptor G5
ADGRG6
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Human
adhesion G protein-coupled receptor G6
ADGRG7
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Human
adhesion G protein-coupled receptor G7
ADGRL1
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Human
adhesion G protein-coupled receptor L1
ADGRL3
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Human
adhesion G protein-coupled receptor L3
ADGRL4
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Human
adhesion G protein-coupled receptor L4
ADGRV1
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Human
adhesion G protein-coupled receptor V1
ADORA1
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Human
adenosine A1 receptor
ADORA2A
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Human
adenosine A2a receptor
ADORA2B
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Human
adenosine A2b receptor
ADORA3
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Human
adenosine A3 receptor
ADRA1A
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Human
adrenoceptor alpha 1A
ADRA1B
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Human
adrenoceptor alpha 1B
ADRA1D
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Human
adrenoceptor alpha 1D
ADRA2A
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Human
adrenoceptor alpha 2A
ADRA2B
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Human
adrenoceptor alpha 2B
ADRA2C
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Human
adrenoceptor alpha 2C
ADRB1
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Human
adrenoceptor beta 1
ADRB2
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Human
adrenoceptor beta 2
ADRB3
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Human
adrenoceptor beta 3
AGTR1
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Human
angiotensin II receptor type 1
AGTR2
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Human
angiotensin II receptor type 2
AKT1
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Human
AKT serine/threonine kinase 1
AKT2
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Human
AKT serine/threonine kinase 2
AKT3
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Human
AKT serine/threonine kinase 3
AP1B1
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Human
adaptor related protein complex 1 subunit beta 1
AP1G1
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Human
adaptor related protein complex 1 subunit gamma 1
AP1G2
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Human
adaptor related protein complex 1 subunit gamma 2
AP1M1
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Human
adaptor related protein complex 1 subunit mu 1
AP1M2
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Human
adaptor related protein complex 1 subunit mu 2
AP1S1
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Human
adaptor related protein complex 1 subunit sigma 1
AP1S2
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Human
adaptor related protein complex 1 subunit sigma 2
AP1S3
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Human
adaptor related protein complex 1 subunit sigma 3
APBB1IP
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Human
amyloid beta precursor protein binding family B member 1 interacting protein
APLNR
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Human
apelin receptor
ARF6
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Human
ADP ribosylation factor 6
ARFIP2
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Human
ADP ribosylation factor interacting protein 2
ARPC1A
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Human
actin related protein 2/3 complex subunit 1A
ARPC1B
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Human
actin related protein 2/3 complex subunit 1B
ARPC2
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Human
actin related protein 2/3 complex subunit 2
ARPC3
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Human
actin related protein 2/3 complex subunit 3
ARPC4
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Human
actin related protein 2/3 complex subunit 4
ARPC5
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Human
actin related protein 2/3 complex subunit 5
ARPC5L
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Human
actin related protein 2/3 complex subunit 5 like
AVPR1A
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Human
arginine vasopressin receptor 1A
AVPR1B
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Human
arginine vasopressin receptor 1B
AVPR2
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Human
arginine vasopressin receptor 2
BCAR1
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Human
BCAR1 scaffold protein, Cas family member
BCL10
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Human
BCL10 immune signaling adaptor
BDKRB1
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Human
bradykinin receptor B1
BDKRB2
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Human
bradykinin receptor B2
BRS3
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Human
bombesin receptor subtype 3
C3AR1
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Human
complement C3a receptor 1
C5AR1
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Human
complement C5a receptor 1
C5AR2
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Human
complement component 5a receptor 2
CALCR
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Human
calcitonin receptor
CALCRL
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Human
calcitonin receptor like receptor
CAMP
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Human
cathelicidin antimicrobial peptide
CARD9
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Human
caspase recruitment domain family member 9
CASR
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Human
calcium sensing receptor
CCKAR
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Human
cholecystokinin A receptor
CCKBR
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Human
cholecystokinin B receptor
CCR1
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Human
C-C motif chemokine receptor 1
CCR10
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Human
C-C motif chemokine receptor 10
CCR2
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Human
C-C motif chemokine receptor 2
CCR3
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Human
C-C motif chemokine receptor 3
CCR4
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Human
C-C motif chemokine receptor 4
CCR5
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Human
C-C motif chemokine receptor 5
CCR6
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Human
C-C motif chemokine receptor 6
CCR7
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Human
C-C motif chemokine receptor 7
CCR8
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Human
C-C motif chemokine receptor 8
CCR9
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Human
C-C motif chemokine receptor 9
CCRL2
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Human
C-C motif chemokine receptor like 2
CD14
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Human
CD14 molecule
CD209
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Human
CD209 molecule
CD36
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Human
CD36 molecule