Ciclosporin

Ciclosporin
Ciclosporin
Systematic (IUPAC) name
(E)-14,17,26,32-tetrabutyl-5-ethyl-8-(1-hydroxy-2-methylhex-4-enyl) -1,3,9,12,15,18,20,23,27-nonamethyl-11,29-dipropyl-1,3,6,9,12,15,18,21,24,27,30- undecaazacyclodotriacontan-2,4,7,10,13,16,19,22,25,28,31-undecaone
Clinical data
Trade names Neoral, Sandimmune
AHFS/Drugs.com monograph
MedlinePlus a601207
Pregnancy cat. C(AU) C(US)
Legal status Prescription Only (S4) (AU) POM (UK) -only (US)
Routes oral, IV, ophthalmic
Pharmacokinetic data
Bioavailability variable
Metabolism hepatic
Half-life variable (about 24 hours)
Excretion biliary
Identifiers
CAS number 59865-13-3 YesY
ATC code L04AD01 S01XA18
PubChem CID 5284373
DrugBank DB00091
ChemSpider 4447449 YesY
UNII 83HN0GTJ6D YesY
KEGG D00184 YesY
ChEMBL CHEMBL160 YesY
Chemical data
Formula C62H111N11O12 
Mol. mass 1202.61
 N(what is this?)  (verify)

Ciclosporin (INN/BAN) (pronounced /ˌskləˈspɔrɪn/),[1] cyclosporine (USAN), cyclosporin (former BAN), or cyclosporin A is an immunosuppressant drug widely used in post-allogeneic organ transplant to reduce the activity of the immune system, and therefore the risk of organ rejection. Initially isolated from the fungus Tolypocladium inflatum isolated from a soil sample obtained by Sandoz scientists at Hardangervidda, Norway in 1969,[2] ciclosporin is a cyclic nonribosomal peptide of 11 amino acids and contains a single D-amino acid, which are rarely encountered in nature.[3]

Contents

Medical uses

The immunosuppressive effect of ciclosporin was discovered on 31 January 1972 by employees of Sandoz (now Novartis) in Basel, Switzerland, in a screening test on immune suppression designed and implemented by Hartmann F. Stähelin, M.D. The success of ciclosporin in preventing organ rejection was shown in kidney transplants by Calne and colleagues at the University of Cambridge,[4] and in liver transplants performed by Dr. Thomas Starzl at the University of Pittsburgh Hospital. The first patient, on 9 March 1980, was a 28-year-old woman.[5] Ciclosporin was subsequently approved for use in 1983.

Apart from in transplant medicine, ciclosporin is also used in psoriasis, severe atopic dermatitis, pyoderma gangrenosum, chronic autoimmune urticaria, and, infrequently, in rheumatoid arthritis and related diseases, although it is only used in severe cases. It is commonly prescribed in the US as an ophthalmic eyedrop for the treatment of dry eyes. It has been investigated for use in many other autoimmune disorders, and is sometimes prescribed in veterinary cases, particularly in extreme cases of immune-mediated hemolytic anemia. Inhaled ciclosporin has been investigated to treat asthma and is being studied as a preventive therapy for chronic rejection of the lungs. Ciclosporin has also been used to help treat patients with ulcerative colitis that do not respond to treatment with steroids.[6] This drug is also used as a treatment of posterior or intermediate uveitis with noninfective etiology.

Ciclosporin has been investigated as a possible neuroprotective agent in conditions such as traumatic brain injury, and has been shown in animal experiments to reduce brain damage associated with injury.[7] Ciclosporin blocks the formation of the mitochondrial permeability transition pore, which has been found to cause much of the damage associated with head injury and neurodegenerative diseases.

Ciclosporin is a drug currently used to experimentally treat cardiac hypertrophy[8][9] (an increase in cell volume). It is a cyclic undecapeptide (chain of 11 amino acid residues) of fungal origin and is used presently as an immunosuppressant.[10]


Cardiac disease

CsA has been shown to decrease cardiac hypertrophy by affecting cardiac myocytes in many ways. CsA binds to CypD to block the opening of MPTP, and thus decreases the release of protein cytochrome C, which can cause programmed cell death.[8][11][12] CypD is a protein within the MPTP that acts as a gate; binding by CsA decreases the amount of inappropriate opening of MPTP, which decreases the intramitochondrial Ca2+.[11] Decreasing intramitochondrial Ca2+ allows for reversal of cardiac hypertrophy caused in the original cardiac response.[11] Decreasing the release of cytochrome C caused decreased cell death during injury and disease.[8] CsA also inhibits the phosphatase calcineurin pathway (14).[8][13][14] Inhibition of this pathway has been shown to decrease myocardial hypertrophy.[9][13][14]

Adverse effects and interactions

Treatment may be associated with a number of potentially serious adverse drug reactions (ADRs).

ADRs can include gingival hyperplasia, convulsions, peptic ulcers, pancreatitis, fever, vomiting, diarrhea, confusion, hypercholesterolemia, dyspnea, numbness and tingling particularly of the lips, pruritus, high blood pressure, potassium retention, and possibly hyperkalemia, kidney and liver dysfunction (nephrotoxicity[15] and hepatotoxicity), burning sensations at finger tips and an increased vulnerability to opportunistic fungal and viral infections.

An alternate form of the drug, cyclosporin G (OG37-324), has been found to be much less nephrotoxic than the standard ciclosporin (cyclosporin A).[16] Cyclosporin G (molecular mass 1217) differs from cyclosporin A in the amino acid 2 position, where an L-norvaline replaces the α-aminobutyric acid.[17]

Mechanism of action

Ciclosporin is thought to bind to the cytosolic protein cyclophilin (immunophilin) of immunocompetent lymphocytes, especially T-lymphocytes. This complex of ciclosporin and cyclophilin inhibits calcineurin, which, under normal circumstances, is responsible for activating the transcription of interleukin 2. In T-cells, activation of the T-cell receptor normally increases intracellular calcium, which acts via calmodulin to activate calcineurin. Calcineurin then dephosphorylates the transcription factor NF-AT (nuclear factor of activated T-cells), which moves to the nucleus of the T-cell and increases the activity of genes coding for IL-2 and related cytokines. Ciclosporin prevents the dephosphorlyation of NF-AT by binding to cyclophilin.[18] It also inhibits lymphokine production and interleukin release and, therefore, leads to a reduced function of effector T-cells. It does not affect cytostatic activity.

Ciclosporin affects mitochondria by preventing the mitochondrial permeability transition pore from opening, thus inhibiting cytochrome c release, a potent apoptotic stimulation factor. This is not the primary mechanism of action for clinical use, but is an important effect for research on apoptosis.

Ciclosporin is believed to elicit its effects by directly binding to the cyclophilin D protein (CypD) that constitutes part of the mitochondrial permeability transition pore (MPTP),[8][11] and by inhibiting the calcineurin phosphatase pathway.[8][10][13] The MPTP is found in the mitochondrial membrane of cardiac myocytes (heart muscle cells) and functions to move calcium ions (Ca2+) into the mitochondria.[8][11] When open, Ca2+ enters the mitochondria, disrupting transmembrane potential (the electric charge across a membrane). If unregulated, this can contribute to mitochondrial swelling and dysfunction.[11] To allow for normal contraction, intracellular Ca2+ increases, and the MPTP in turn opens, shuttling Ca2+ into the mitochondria.[11] Calcineurin is a Ca2+-activated phosphatase (enzyme that removes a phosphate group from substrate) that regulates cardiac hypertrophy.[9][13][14] Regulation occurs through NFAT (nuclear factor of activated T-cells) activation, which, when dephosphorylated, binds to GATA and forms a transcription factor (protein that can bind DNA and alter the expression of DNA) with ability to control the hypertrophic gene (2). Activation of calcineurin causes increases in hypertrophy.[9][13]

Biosynthesis

Figure 1: Ciclosporin biosynthesis. Bmt = butenyl-methyl-threonine, Abu = L-alpha-aminobutyric acid, Sar = sarcosine

Ciclosporin is synthesized by a nonribosomal peptide synthetase, ciclosporin synthetase. The enzyme contains an adenylation domain, a thiolation domain, a condensation domain, and an N-methyltransferase[disambiguation needed ] domain. The adenylation domain is responsible for substrate recognition and activation, whereas the thiolation domain covalently binds the adenylated amino acids to phosphopantetheine, and the condensation domain elongates the peptide chain. Ciclosporin synthetase substrates include L-valine, L-leucine, L-alanine, L-glycine, 2-aminobutyric acid, 4-methylthreonine, and D-alanine. With the adenylation domain, ciclosporin synthetase generates the acyl-adenylated amino acids, then covalently binds the amino acid to phosphopantetheine through a thioester linkage. Some of the amino acid substrates become N-methylated by S-adenosyl methionine. The cyclization step releases ciclosporin from the enzyme.[19] Amino acids such as D-Ala and butenyl-methyl-L-threonine indicate ciclosporin synthetase requires the action of other enzymes such as a D-alanine racemase. The racemization of L-Ala to D-Ala is pyridoxal phosphate-dependent. The formation of butenyl-methyl-L-threonine is performed by a butenyl-methyl-L-threonine polyketide synthase that uses acetate/malonate as its starting material.[20]

Figure 2: Butenyl-methyl-L-Threonine biosynthesis


Cardiac disease

Inappropriate opening of the mitochondrial permeability transition pore (MPTP) manifests in ischemia[8] (blood flow restriction to tissue) and reperfusion injury[8] (damage occurring after ischemia when blood flow returns to tissue), after myocardial infarction[13] (heart attack) and when mutations in mitochondrial DNA polymerase occur.[8] The heart attempts to compensate for disease state by increasing the intracellular Ca2+ to increase the contractility cycling rates.[11] Constitutively high levels of mitochondrial Ca2+ cause inappropriate MPTP opening leading to a decrease in the cardiac range of function, leading to cardiac hypertrophy as an attempt to compensate for the problem.[11][13]

Formulations

The drug exhibits very poor solubility in water, and, as a consequence, suspension and emulsion forms of the drug have been developed for oral administration and for injection. Ciclosporin was originally brought to market by Sandoz, now Novartis, under the brand name Sandimmune, which is available as soft gelatin capsules, as an oral solution, and as a formulation for intravenous administration. These are all nonaqueous compositions.[21] A newer microemulsion, orally-administered formulation, Neoral,[22] is available as a solution and as soft gelatin capsules. The Neoral compositions are designed to form microemulsions in contact with water. Generic ciclosporin preparations have been marketed under various trade names, including Cicloral (Sandoz/Hexal), Gengraf (Abbott)and Deximune (Dexcel Pharma Ltd). Since 2002, a topical emulsion of ciclosporin for treating inflammation caused by keratoconjunctivitis sicca (dry eye syndrome) has been marketed under the trade name Restasis (0.05%). Inhaled ciclosporin formulations are in clinical development, and include a solution in propylene glycol and liposome dispersions.

The drug is also available in a dog preparation manufactured by Novartis Animal Health called Atopica. Atopica is indicated for the treatment of atopic dermatitis in dogs. Unlike the human form of the drug, the lower doses used in dogs mean the drug acts as an immunomodulator and has fewer side effects than in humans. The benefits of using this product include the reduced need for concurrent therapies to bring the condition under control. It is available as an ophthalmic ointment for dogs called Optimmune, manufactured by Intervet, which is part of Merck.

See also

References

  1. ^ "cyclosporin". Dictionary.com Unabridged. Random House. [n.d.]. http://dictionary.reference.com/browse/cyclosporin. Retrieved 2011-07-13. 
  2. ^ Wu AH (January 1989). "Creatine kinase isoforms in ischemic heart disease". Clin. Chem. 35 (1): 7–13. PMID 2642764. http://www.clinchem.org/cgi/pmidlookup?view=long&pmid=2642764. 
  3. ^ Borel JF (2002). "History of the discovery of cyclosporin and of its early pharmacological development". Wien. Klin. Wochenschr. 114 (12): 433–7. PMID 12422576. 
    Some sources list the fungus under an alternative species name Hypocladium inflatum gams such as Pritchard and Sneader in 2005:
    * Pritchard DI (2005). "Sourcing a chemical succession for cyclosporin from parasites and human pathogens". Drug Discov. Today 10 (10): 688–91. doi:10.1016/S1359-6446(05)03395-7. PMID 15896681. 
    * "Ciclosporin". Drug Discovery — A History. John Wiley & Sons. pp. 298–299 (refs. page 315). 
    However, the name, "Beauveria nivea", also appears in several other articles including in a 2001 online publication by Harriet Upton entitled "Origin of drugs in current use: the cyclosporin story" (retrieved June 19, 2005). Mark Plotkin states in his book Medicine Quest, Penguin Books 2001, pages 46-47, that in 1996 mycology researcher Kathie Hodge found that it is in fact a species of Cordyceps.
  4. ^ Calne RY, White DJG, Thiru S, Evans DB, McMaster P, Dunn DC, et al. Cyclosporin A in patients receiving renal allografts from cadaver donors. The Lancet 1978/II:1323-1327
  5. ^ Starzl TE, Klintmalm GB, Porter KA, Iwatsuki S, Schröter GP (1981). "Liver transplantation with use of cyclosporin a and prednisone". N. Engl. J. Med. 305 (5): 266–9. doi:10.1056/NEJM198107303050507. PMC 2772056. PMID 7017414. http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pmcentrez&artid=2772056. 
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  9. ^ a b c d Mende U, Kagen A, Cohen A, Aramburu J, Schoen FJ, Neer EJ (November 1998). "Transient cardiac expression of constitutively active Galphaq leads to hypertrophy and dilated cardiomyopathy by calcineurin-dependent and independent pathways". Proc. Natl. Acad. Sci. U.S.A. 95 (23): 13893–8. doi:10.1073/pnas.95.23.13893. PMC 24952. PMID 9811897. http://www.pnas.org/cgi/pmidlookup?view=long&pmid=9811897. 
  10. ^ a b Handschumacher RE, Harding MW, Rice J, Drugge RJ, Speicher DW (November 1984). "Cyclophilin: a specific cytosolic binding protein for cyclosporin A". Science 226 (4674): 544–7. doi:10.1126/science.6238408. PMID 6238408. http://www.sciencemag.org/cgi/pmidlookup?view=long&pmid=6238408. 
  11. ^ a b c d e f g h i Elrod JW, Wong R, Mishra S, et al. (October 2010). "Cyclophilin D controls mitochondrial pore-dependent Ca2+ exchange, metabolic flexibility, and propensity for heart failure in mice". J. Clin. Invest. 120 (10): 3680–7. doi:10.1172/JCI43171. PMC 2947235. PMID 20890047. http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pmcentrez&artid=2947235. 
  12. ^ Wilkinson ST, Johnson DB, Tardif HL, Tome ME, Briehl MM (2010). "Increased cytochrome c correlates with poor survival in aggressive lymphoma". Oncol Lett 1 (2): 227–230. doi:10.3892/ol_00000040. PMC 2927837. PMID 20798784. http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pmcentrez&artid=2927837. 
  13. ^ a b c d e f g Youn TJ, Piao H, Kwon JS, et al. (December 2002). "Effects of the calcineurin dependent signaling pathway inhibition by cyclosporin A on early and late cardiac remodeling following myocardial infarction". Eur. J. Heart Fail. 4 (6): 713–8. doi:10.1016/S1388-9842(02)00120-4. PMID 12453541. http://eurjhf.oxfordjournals.org/cgi/pmidlookup?view=long&pmid=12453541. 
  14. ^ a b c Lim HW, De Windt LJ, Mante J, et al. (April 2000). "Reversal of cardiac hypertrophy in transgenic disease models by calcineurin inhibition". J. Mol. Cell. Cardiol. 32 (4): 697–709. doi:10.1006/jmcc.2000.1113. PMID 10756124. http://linkinghub.elsevier.com/retrieve/pii/S0022-2828(00)91113-1. 
  15. ^ Naesens M, Kuypers DR, Sarwal M (2009). "Calcineurin inhibitor nephrotoxicity". Clin. J. Am. Soc. Nephrol. 4 (2): 481–509. doi:10.2215/CJN.04800908. PMID 19218475. 
  16. ^ Henry ML, Elkhammas EA, Davies EA, Ferguson RM (1995). "A clinical trial of cyclosporine G in cadaveric renal transplantation". Pediatr. Nephrol. 9 (Suppl): S49–51. doi:10.1007/BF00867684. PMID 7492487. 
  17. ^ Calne RY, White DJ, Thiru S, Rolles K, Drakopoulos S, Jamieson NV (1985). "Cyclosporin G: immunosuppressive effect in dogs with renal allografts". Lancet 1 (8441): 1342. doi:10.1016/S0140-6736(85)92844-2. PMID 2860538. 
  18. ^ William F. Ganong. Review of medical physiology, 22nd edition, Lange medical books, chapter 27, page 530. ISBN 0-07-144040-2
  19. ^ Hoppert M, Gentzsch C, Schörgendorfer K (October 2001). "Structure and localization of cyclosporin synthetase, the key enzyme of cyclosporin biosynthesis in Tolypocladium inflatum". Arch. Microbiol. 176 (4): 285–93. doi:10.1007/s002030100324. PMID 11685373. http://link.springer.de/link/service/journals/00203/papers/1176004/11760285.pdf. 
  20. ^ Dewick, P. (2001) Medicinal Natural Products. John Wiley & Sons, Ltd. 2nd ed.
  21. ^ http://www.pharma.us.novartis.com/product/pi/pdf/sandimmune.pdf
  22. ^ http://www.pharma.us.novartis.com/product/pi/pdf/neoral.pdf

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