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HOW I USE METHOTREXATE IN CHILDREN?
RCIAPCON 2005

T. P. Yadav

METHOTREXATE
  • FOLIC ACID ANALOGUE
  • ANTI-INFLAMMATORY
  • ANTI-METABOLITE
  • IMMUNO-MODULATOR
  • ?a ADENOSINELEVELS
    - INHIBITS NEUTRO-ADHERENCE
  • INHIBITS PROLIFERATION OF
    SYNOVIAL CELLS
  • INHIBITS CMI
INHIBITS ENZYMES
  • DIHYDROFOLATE REDUCTASE
  • 5. AMINOIMIDAZOLE – 4 – CARBOXANIDE RIBO NUCLEOTIDE TRANSFORMYLASE
  • THYMIDYLATE SYNTHETASE
  • ADENOSINE DEAMINASE
KINETICS
  • 50-70% Abs – ORAL Admn
  • PLASMA HALF LIFE – 2 Hrs
  • TRIPHASIC PHARMACOKINETICS
    - BLOOD LEVELS ASSAY
    - LATENT PERIOD OF WEEKS
    - PROBABLY TRUE ANTI-INFLAM
  • 80% eliminated by kidneys within 8-48 Hrs.
  • 11-57% Protein bound at low doses.
  • Oral MTX abs. – saturable process, SC is not.
METHOTREXATE IN CHILDREN
  • WHERE & WHEN TO USE
  • HOW TO USE
  • SAFETY ISSUES
  • MONITORING
  • HOW LONG TO USE
  • WHEN TO DISCONTINUE
WHERE & WHEN
  • JIA – POLYARTICULAR
    - EXTENDED PAUCI
    - SOJIA
    - ERA
    - JPsA
  • JDMS “ Steroid non responsive
  • SLE
  • SARCOIDOSIS
  • SCLERODERMA
HOW TO USE
  • DOSE – 10-15 mg/kg/wk
    Or 0.3 – 0.6 mg/kg/wk (20-25 mg/m2/wk, 1.1 mg/kg/wk)
  • ROUTE Oral – empty stomach
    - With clear liquids
    - Or 1 Hr before BF Parenteral – SC, IM, IV
  • Availability – Tablets 2.5, 5, 7.3, 10 mg Inj 15 mg/ml
PARENTERAL MTX
  • Patients with poor clinical response to oral MTX
  • Need a dose in excess of 15 mg/m2/wk
  • Develop significant GI Toxicity with oral MTX
  • Is SC better than Oral ?
  • Folic acid-to give or not ?
  • Avoid in renal insufficiency.
SIDE EFFECTS
  • GIT – Nausea, vomiting, ulceration, diarrhea
  • Haematological – Bone marrow suppression cytopenia
  • Hepatic – Raised enzymes (9%), Fibrosis?
  • Alopecia, Dermatitis
  • Renal
  • Risk of infection
  • Oncogenicity, Gonadal dysfunction, Nodulosis
  • Teratogenicity
MONITORING
BASELINE –

Wt, Ht Surface Area
  - CBC, UA, LFT, KFT, S.protein
  - ESR, CRP
      Clinical – global assessment
        - No of Active joints / joints with limited ROM
         - Duration of morning stiffness
After Starting MTX – Initially Lab – every 2 wks x 3 mths.
then every 1-3 mths
Clinical 1-3 mth.

MONITORING
  • DISCONTINUE / REDUCE> 3 TIMES UPPER N LIMIT
  • FULL BLOOD COUNT       Platelets <150 x 109/L
          WBC <3.5 x 109xL
          Neutrophils <1.5x109L
* Rash/Severe oral ulcers/new or increasing dyspnoea or cough

DURATION / DISCONTINUATION

MTX-GIVE FOR 3-6 MONTHS
RESPONSE-CONTINUE
IF NO RESPONSE-I DOSE/

CHANGE ROUTE 3-6 MONTHS
IF STILL NO RESPONSE-CHANGE
No VALIDATED GUIDELINES FOR DURATION
- Clinical remission for 1 year
- Disease Flare in more than 50%

R M L H Experience

MTX TOTAL NO OF PATIENTS
ANALYSED 24+2
POLY JIA = 10,
SOJIA = 12
EXTENDED PAUCI = 2

-

POLY (n = 10)

SOJIA (n = 12)

AGE (yr)

5-12

3.5-10

DIS. DURATION (yr)

1-6 (3.25 ± 1.75

2-4.5 (3.3 ± 1.3)

DUR. MTX (WK)

60-208 (104 ± 64)

16-162 (86 ± 70)

ROUTE

ORAL / SC-2

ORAL

RESPONSE

- -

COMPLETE

5 2

PARTIAL

3 6

NONE

2 3

SIDE EFFECTS

Nausea –2, Vom 2

Pn., boils

OTHER DRUGS

NSAID, SSZ

NSAID, STRD.


Last Updated on 15-06-2006

How to cite this url
RCIAPCON 2005 - Conference Abstracts.Pediatric Oncall [serial online] 2006 [cited 15 June 2006(Supplement 6)];3. Available from:
http://www.pediatriconcall.com/fordoctor/Conference_abstracts/
METHOTREXATE_IN_CHILDREN.asp
 
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