Alternative complement pathway explained

The alternative pathway is a type of cascade reaction of the complement system and is a component of the innate immune system, a natural defense against infections.

The alternative pathway is one of three complement pathways that opsonize and kill pathogens. The pathway is triggered when the C3b protein directly binds a microbe. It can also be triggered by foreign materials and damaged tissues.

Cascade

This change in shape allows the binding of plasma protein Factor B, which allows Factor D to cleave Factor B into Ba and Bb.

Bb remains bound to C3(H2O) to form C3(H2O)Bb. This complex is also known as a fluid-phase C3-convertase. This convertase, the alternative pathway C3-convertase, although only produced in small amounts, can cleave multiple C3 proteins into C3a and C3b. The complex is believed to be unstable until it binds properdin, a serum protein. The addition of properdin forms the complex C3bBbP, a stable compound which can bind an additional C3b to form alternative pathway C5-convertase.

The C5-convertase of the alternative pathway consists of (C3b)2BbP (sometimes referred to as C3b2Bb). After the creation of C5 convertase (either as (C3b)2BbP or C4b2a3b from the classical pathway), the complement system follows the same path regardless of the means of activation (alternative, classical, or lectin). C5-convertase cleaves C5 into C5a and C5b. C5b binds sequentially to C6, C7, C8 and then to multiple molecules of C9 to form membrane attack complex.

Regulation

Since C3b is free and abundant in the plasma, it can bind to either a host cell or a pathogen surface. To prevent complement activation from proceeding on the host cell, there are several different kinds of regulatory proteins that disrupt the complement activation process:

Role in disease

Dysregulation of the complement system has been implicated in several diseases and pathologies, including atypical hemolytic uremic syndrome in which kidney function is compromised. Age related macular degeneration (AMD) is now believed to be caused, at least in part, by complement overactivation in retinal tissues.[5] Alternative pathway activation also plays a significant role in complement-mediated renal disorders such as atypical hemolytic uremic syndrome, C3 glomerulopathy, and C3 glomerulonephritis (Dense Deposit Disease or MPGN Type II).

See also

Further reading

Notes and References

  1. Conrad DH, Carlo JR, Ruddy S . Interaction of beta1H globulin with cell-bound C3b: quantitative analysis of binding and influence of alternative pathway components on binding . The Journal of Experimental Medicine . 147 . 6 . 1792–1805 . June 1978 . 567241 . 2184316 . 10.1084/jem.147.6.1792 .
  2. Weiler JM, Daha MR, Austen KF, Fearon DT . Control of the amplification convertase of complement by the plasma protein beta1H . Proceedings of the National Academy of Sciences of the United States of America . 73 . 9 . 3268–72 . September 1976 . 1067618 . 431003 . 10.1073/pnas.73.9.3268 . 1976PNAS...73.3268W . free .
  3. Pangburn MK, Schreiber RD, Müller-Eberhard HJ . Human complement C3b inactivator: isolation, characterization, and demonstration of an absolute requirement for the serum protein beta1H for cleavage of C3b and C4b in solution . The Journal of Experimental Medicine . 146 . 1 . 257–70 . July 1977 . 301546 . 2180748 . 10.1084/jem.146.1.257 .
  4. McRae JL, Duthy TG, Griggs KM, Ormsby RJ, Cowan PJ, Cromer BA, McKinstry WJ, Parker MW, Murphy BF, Gordon DL . Human factor H-related protein 5 has cofactor activity, inhibits C3 convertase activity, binds heparin and C-reactive protein, and associates with lipoprotein . Journal of Immunology . 174 . 10 . 6250–6 . May 2005 . 15879123 . 10.4049/jimmunol.174.10.6250 . free .
  5. Tzoumas. Nikolaos. Hallam. Dean. Harris. Claire L.. Lako. Majlinda. Kavanagh. David. Steel. David H.W.. November 2020. Revisiting the role of factor H in age-related macular degeneration: Insights from complement-mediated renal disease and rare genetic variants. Survey of Ophthalmology. 66. 2. 378–401. 10.1016/j.survophthal.2020.10.008. 33157112. 226274874. 0039-6257.