79217-60-0
Name | CYCLOSPORINE |
CAS | 79217-60-0 |
EINECS(EC#) | 1312995-182-4 |
Molecular Formula | C62H111N11O12 |
MDL Number | MFCD01771104 |
Molecular Weight | 1202.61 |
MOL File | 79217-60-0.mol |
Synonyms
CYCLOSPORIN
CYCLOSPORINE
Cyclosporin A/B/C/D/H A 59865-13-3 /
Cyclosporins
CYCLOSPRINE
CYCLOSPORINE/CICLOSPORIN
Chemical Properties
Appearance | White crystalline solid or powder. |
form | Solid |
color | White to light yellow |
BCS Class | 2,3,4 |
CAS DataBase Reference | 79217-60-0(CAS DataBase Reference) |
IARC | 1 (Vol. 50, 100A) 2012 |
Hazard Information
Potential Exposure
Cyclosporin A is a fungal metabolite;
an amide immunosuppressant drug used in various
surgeries.
First aid
Skin Contact
: Flood all areas of body that
have contacted the substance with water. Don’t wait to
remove contaminated clothing; do it under the water
stream. Use soap to help assure removal. Isolate contami-
nated clothing when removed to prevent contact by others.
Eye Contact: Remove any contact lenses at once. Flush
eyes well with copious quantities of water or normal saline
for at least 20 30 minutes. Seek medical attention.
Inhalation: Leave contaminated area immediately; breathe
fresh air. Proper respiratory protection must be supplied to
any rescuers. If coughing, difficult breathing, or any other
symptoms develop, seek medical attention at once, even if
symptoms develop many hours after exposure. Ingestion: If
convulsions are not present, give a glass or two of water or
milk to dilute the substance. Assure that the person’s air-
way is unobstructed and contact a hospital or poison center
immediately for advice on whether or not to induce
vomiting.
Shipping
UN3249 Medicine, solid, toxic, n.o.s., Hazard
Class: 6.1; Labels: 6.1-Poisonous materials.
Incompatibilities
Amides/imides react with azo and diazo
compounds to generate toxic gases. Flammable gases are
formed by the reaction of organic amides/imides with
strong reducing agents such as hydrideds and active metals.
Amides are very weak bases (weaker than water). Imides
are less basic yet and in fact react with strong bases to
form salts. That is, they can react as acids. Mixing amides
with dehydrating agents such as such as phosphorus pent-
oxide or thionyl chloride generates the corresponding
nitrile. The combustion of these compounds generates
mixed oxides of nitrogen (NOx).
Description
Cyclosporine is a cyclic polypeptide with potent, partially selective immunosupressive
activity. Isolated from the species Cylindrocarpon lucidium and
Trichoderma polysporum, cyclosporine is useful in the prevention and treatment
of graft/host disease and the prevention of rejection following organ transplantation.
It appears to act by preferentially suppressing T-lymphocytes.
Cyclosporine lacks myelotoxicity, although impaired renal and liver function have
been observed. Initial administration is via the intravenous route, followed by
oral maintenance therapy.
Chemical Properties
White crystalline solid or powder.
Waste Disposal
t is inappropriate and possibly
dangerous to the environment to dispose of expired or waste
drugs and pharmaceuticals by flushing them down the toilet
or discarding them to the trash. Household quantities of
expired or waste pharmaceuticals may be mixed with wet
cat litter or coffee grounds, double-bagged in plastic, discard
in trash. Larger quantities shall carefully take into consider-
ation applicable DEA, EPA, and FDA regulations. If possi-
ble return the pharmaceutical to the manufacturer for proper
disposal being careful to properly label and securely package
the material. Alternatively, the waste pharmaceutical shall be
labeled, securely packaged, and transported by a state
licensed medical waste contractor to dispose by burial in a
licensed hazardous or toxic waste landfill or incinerator.
Originator
Sandoz (Switzerland)
Indications
Cyclosporine (Sandimmune) is a potent inhibitor of antibody-
and cell-mediated immune responses and is the
immunosuppressant of choice for the prevention of
transplant rejection. It also has application in the treatment
of autoimmune diseases.
Cyclosporine is a highly stable 11-amino acid cyclic polypeptide. The molecule is very lipophilic and essentially is not soluble in water. It can be administered intravenously, orally, or by injection.
Cyclosporine is a highly stable 11-amino acid cyclic polypeptide. The molecule is very lipophilic and essentially is not soluble in water. It can be administered intravenously, orally, or by injection.
Brand name
SANDIMMUN
Mechanism of action
Cyclosporine can bind to the cytosolic protein cytophilin
C. This drug–protein complex inhibits calcineurin
phosphatase activity, which leads to a decreased
synthesis and release of several cytokines,
including interleukins IL-2, IL-3, IL-4, interferon-, and
tumor necrosis factor.
Cyclosporine exhibits a high degree of specificity in its actions on T cells without significantly impairing Bcell activity. It can inhibit the T cell–dependent limb of antibody production by lymphocytes by preventing the differentiation of B cells into antibody-secreting plasma cells. Because T cells appear to require IL-2 stimulation for their continuous growth, cyclosporine impairs the proliferative response of T cells to antigens. However, once T cells have been stimulated by antigens to synthesize IL-2, cyclosporine cannot suppress the proliferation of T cells induced by this cytokine.
Cyclosporine exhibits a high degree of specificity in its actions on T cells without significantly impairing Bcell activity. It can inhibit the T cell–dependent limb of antibody production by lymphocytes by preventing the differentiation of B cells into antibody-secreting plasma cells. Because T cells appear to require IL-2 stimulation for their continuous growth, cyclosporine impairs the proliferative response of T cells to antigens. However, once T cells have been stimulated by antigens to synthesize IL-2, cyclosporine cannot suppress the proliferation of T cells induced by this cytokine.
Pharmacology
After oral administration, cyclosporine is absorbed
slowly and incompletely, with great variation among individuals.
Peak plasma concentrations are reached in
3 to 4 hours, and the plasma half-life is 10 to 27 hours.
The drug is extensively metabolized by hepatic mixedfunction
oxidase enzymes and is excreted principally via
the bile into the feces. Metabolism results in inactivation
of the immunosuppressive activity.Agents that enhance
or inhibit the mixed-function oxidase enzymes
will alter the therapeutic response to cyclosporine.
Clinical Use
Cyclosporine has been approved for use in allogeneic
kidney, liver, and heart transplant patients and is under
study for use in pancreas, bone marrow, single lung, and
heart–lung transplant procedures. It is recommended
that corticosteroids, such as prednisone, be used concomitantly,
although at half or less of their usual dose.
Such combined therapy leads to fewer side effects, a decreased
incidence of infectious complications, efficacy
of lower doses of cyclosporine, and a better history of
patient survival.
Cyclosporine appears to have promise in the treatment of autoimmune diseases. It has a beneficial effect on the course of rheumatoid arthritis, uveitis, insulindependent diabetes, systemic lupus erythematosus, and psoriatic arthropathies in some patients. Toxicity is more of a problem in these conditions than during use in transplantation, since higher doses of cyclosporine are often required to suppress autoimmune disorders.
Cyclosporine appears to have promise in the treatment of autoimmune diseases. It has a beneficial effect on the course of rheumatoid arthritis, uveitis, insulindependent diabetes, systemic lupus erythematosus, and psoriatic arthropathies in some patients. Toxicity is more of a problem in these conditions than during use in transplantation, since higher doses of cyclosporine are often required to suppress autoimmune disorders.
Side effects
Compared with previously available therapy, the adverse
effects associated with cyclosporine are much less severe
but still worthy of concern. Nephrotoxicity, which can occur
in up to 75% of patients, ranges from severe tubular
necrosis to chronic interstitial nephropathy.This effect is
generally reversible with dosage reduction. Vasoconstriction
appears to be an important aspect of cyclosporine-
induced nephrotoxicity. Hypertension occurs in
25% of the patients and more frequently in patients with
some degree of renal dysfunction; the concomitant use of
antihypertensive drugs may prove useful. Hyperglycemia,
hyperlipidemia, transient liver dysfunction, and
unwanted hair growth are also observed.
Veterinary Drugs and Treatments
Cyclosporine may be useful as an immunosuppressant for immunemediated
diseases
(see dosage section) and as part of a protocol to
reduce the rejection of allografts in transplant medicine in dogs and
cats.
Questions And Answer
-
Application in Particular Diseases
In Rheumatic Arthritis:
Cyclosporine reduces production of cytokines involved in T-cell activation and has direct effects on B cells, macrophages, bone, and cartilage cells. Its onset appears to be 1 to 3 months. Important toxicities at doses of 1 to 10 mg/kg/day include hypertension, hyperglycemia, nephrotoxicity, tremor, GI intolerance, hirsutism, and gingival hyperplasia. Cyclosporine should be reserved for patients refractory to or intolerant of other DMARDs. It should be avoided in patients with current or past malignancy, uncontrolled hypertension, renal dysfunction, immunodeficiency, low white blood cell or platelet counts, or elevated liver function tests. ;
Supplier
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