I'm back. I'm awful with computers. I posted several times in September and everyone was very kind. Thank you. We changed internet companies and it has been a nightmare!! Can someone "send" me to a place I can find out about Prednisone and Methotrexate? Can one or both cause the bones to thin and break easily? Thanks!!! Nana1.Ask this question in the RA section of the message board.
http://www.arthritisinsight.com/forum/forum_topics.asp?FID=8
I've read that Prednisone can cause this affect.
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Methotrexate | |
| Systematic (IUPAC) name | |
| (S)-2-(4-(((2,4-diaminopteridin-6-yl) methyl)methylamino)benzamido) pentanedioic acid | |
| Identifiers | |
| CAS number | 59-05-2 |
| ATC code | L01BA01 L04AX03 |
| PubChem | 126941 |
| DrugBank | APRD00353 |
| Chemical data | |
| Formula | C20H22N8O5 |
| Mol. mass | 454.44 g/mol |
| Pharmacokinetic data | |
| Bioavailability | 17–90% |
| Metabolism | hepatic |
| Half life | 3–15 hours (dose dependent) |
| Excretion | renal 48–100% |
| Therapeutic considerations | |
| Pregnancy cat. | |
| Legal status | |
| Routes | oral, IV, IM, SC, intrathecal |
Methotrexate (rINN) (IPA: [mɛèəˈtrɛkseɪt]), abbreviated MTX and formerly known as amethopterin, is an antimetabolite and antifolate drug used in treatment of cancer and autoimmune diseases. It acts by inhibiting the metabolism of folic acid. Methotrexate replaced the more powerful and toxic antifolate aminopterin, and the two should not be confused with each other.
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Methotrexate originated in the 1940s when Dr.Sidney Farber at Chief of Pathology Department at Children's Hospital Boston was testing the effects of folic acid on Acute leukemic children ( severe blood cancer). Then inspired and requested the team leader Dr. Yellapragada Subbarow, the Director, Research Division, Lederle Labs of American Cyanamid Company, Pearl river, NY., ( a person of Indian origin and former faculty at Harvard Medical school and a colleague of Dr Farber) and his team to synthesiz ethe anti-folate (Methotrexate). The team which had earlier synthesized Folic acid (1946) readily synthesized this anti-folate and handed it over to Dr. Farber, who in turn administered it to a small group of very ill leukemic children. A remarkable clinical improvement observed in these kids heralded the era of first ever cancer chemotherapy in Modern Medicine. Dr. S. Farber, in 1950, founded in Boston, the first ever Cancer Research Center in the world. Methotrexate gained Food and Drug Administration (FDA) approval as an oncology drug in 1953.
Methotrexate was originally used, as part of combination chemotherapy regimens, to treat many kinds of cancers. It is still the mainstay for the treatment of many neoplastic disorders including acute lymphoblastic leukemia.
More recently it has come into use as a treatment for some autoimmune diseases, including ankylosing spondylitis, Crohn's disease, psoriasis, psoriatic arthritis, and rheumatoid arthritis (see disease-modifying antirheumatic drugs). A parallel use with TNFá blockers as infliximab or etanercept has been shown to markedly improve symptoms.[1]
Although not indicated for this use, methotrexate is also sometimes used (generally in combination with misoprostol) to terminate early pregnancies, particularly ectopic pregnancies.
Methotrexate is a weak dicarboxylic acid with pKa 4.8 and 5.5, and thus it is mostly ionized at physiologic pH. Oral absorption is saturatable and thus dose-dependent, with doses less than 40mg/M2 having 42% bioavailability and doses greater than 40mg/M2 only 18%. Mean oral bioavailability is 33% (13-76% range), and there is no clear benefit to subdividing an oral dose. Mean intramuscular bioavailability is 76%.
Methotrexate is metabolized by intestinal bacteria to the inactive metabolite 4-amino-4-deoxy-N-methylpteroic acid (DAMPA) and accounts for less than 5% loss of the oral dose.
Factors that decrease absorption include food, oral non-absorbable antibiotics (e.g. vancomycin, neomycin, and bacitracin), and more rapid transit through the Gastrointestinal (GI) tract such as diarrhea, while slower transit time in the GI tract from constipation will increase absorption.
It can be taken orally or administered by injection (subcutaneous, intramuscular, intravenous or intrathecal). Although daily preparations are occasionally used, most patients take weekly doses, which decreases the risk of certain side-effects.
Possible side effects can include anemia, neutropenia, increased risk of bruising, nausea and vomiting, dermatitis and diarrhea. A small percentage of patients develop hepatitis, and there is an increased risk of pulmonary fibrosis.
The higher doses of methotrexate often used in cancer chemotherapy can cause toxic effects to the rapidly-dividing cells of bone marrow and gastrointestinal mucosa. The resulting myelosuppression and mucositis are often prevented (termed methotrexate "rescue") by using folinic acid supplements (not to be confused with folic acid).
Methotrexate is a highly teratogenic drug and categorized in Pregnancy Category X by the FDA. Women must not take the drug during pregnancy, if there is a risk of becoming pregnant, or if they are breastfeeding. Men who are trying to get their partner pregnant must also not take the drug. To engage in any of these activities (after discontinuing the drug), women must wait until the end of a full ovulation cycle and men must wait three months.
There is a risk of a severe adverse reaction if penicillin is prescribed alongside methotrexate.
Interestingly, there have also been some reports of central nervous system reactions to methotrexate especially when given via the intrathecal route which include myelopathies and leucoencephalopathies.
Methotrexate competitively and reversibly inhibits dihydrofolate reductase (DHFR), an enzyme that is part of the folate synthesis metabolic pathway. The affinity of methotrexate for DHFR is about one thousand-fold that of folate for DHFR. Dihydrofolate reductase catalyses the conversion of dihydrofolate to the active tetrahydrofolate. Folic acid is needed for the de novo synthesis of the nucleoside thymidine, required for DNA synthesis. Also, folate is needed for purine base synthesis, so all purine synthesis will be inhibited. Methotrexate, therefore, inhibits the synthesis of DNA, RNA, thymidylates, and proteins.
Methotrexate acts specifically during DNA and RNA synthesis, and thus it is cytotoxic during the S-phase of the cell cycle. Logically, it therefore has a greater toxic effect on rapidly dividing cells (such as malignant and myeloid cells, and GI & oral mucosa), which replicate their DNA more frequently, and thus inhibits the growth and proliferation of these non-cancerous cells as well causing side effects listed above.
Lower doses of methotrexate have been shown to be very effective for the management of rheumatoid arthritis and psoriasis. In these cases inhibition of dihydrofolate reductase (DHFR) is not thought to be the main mechanism, rather the inhibition of enzymes involved in purine metabolism, leading to accumulation of adenosine, or the inhibition of T cell activation and suppression of intercellular adhesion molecule expression by T cells.[2]