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Topical Immunosuppressants

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Title: Topical Immunosuppressants


1
Topical Immunosuppressants
  • Bindi M. Nikhar, M.D., FAAP
  • Division of Dermatologic and Dental Drug
    Products, ODE V

2
TOPICAL IMMUNOSUPPRESSANTS
  • Newest pharmacological class for AD
  • Introduced in this decade
  • Direct immunosuppressive action in diseases with
    an immunological basis
  • 2 currently FDA approved products
  • Tacrolimus (FK506) (trade name Protopic)
  • Pimecrolimus (SDZ ASM 981) (trade name Elidel)

3
Background
  • Tacrolimus ointment approved on 12/08/2000, 0.03
    ointment approved for children 2 to 15 years,
    0.1 ointment approved for adults.
  • Indication in both age groups is short and
    intermittent long term therapy of patients with
    moderate to severe AD.
  • Systemic Tacrolimus (Prograf) first introduced
    for prevention of allograft rejection, now used
    in kidney, liver and heart transplantation

4
Background (contd)
  • Elidel cream 1 approved on 12/13/2001.
  • Indicated for patients 2 years of age and older
    for short and intermittent long term therapy in
    the treatment of mild to moderate atopic
    dermatitis.
  • Both drugs not approved for use in children less
    than 2 years of age.
  • Systemic absorption can take place in both adult
    and pediatric age groups from the topical
    application of both drugs.
  • Currently, the effects of topical
    immunosuppressants on the developing immune
    system are unknown.

5
Pharmacokinetic (PK) studies for Tacrolimus
  • Pooled results from 2 PK studies in 49 adult
    moderate-severe AD patients indicate that
    tacrolimus is absorbed after the topical
    application of 0.1 Protopic ointment.
  • Peak tacrolimus levels ranged from undetectable
    to 20 ng/ml after single or multiple doses of
    0.1 Protopic ointment, 45 out of the 49 patients
    had peak concentrations less than 5 ng/ml.

6
Pharmacokinetic studies for Tacrolimus (contd)
  • A PK study of 0.1 Protopic ointment in 20
    pediatric AD patients (ages 6-13 years), showed
    peak tacrolimus concentrations below 1.6 ng/ml in
    all patients.
  • Absolute bioavailability of topical tacrolimus is
    unknown.
  • Using iv historical data for comparison, the
    bioavailability of tacrolimus from Protopic in AD
    patients is lt 0.5.
  • Lowest tacrolimus blood level at which systemic
    effects can be observed is not known.

7
Pharmacokinetic studies for Pimecrolimus
  • In adults treated for AD with 1362 BSA
    involvement for periods up to a year, detectable
    pimecrolimus blood concentrations were lt 2 ng/ml
    (LOQ lt0.5 ng/ml).
  • In 26 pediatric patients between 2-14 years with
    AD (20-69 BSA involvement) who had b.i.d.
    application for 3 weeks, blood concentrations of
    pimecrolimus were lt 3 ng/ml (LOQ lt 0.5 ng/ml)

8
Pharmacokinetic studies for Pimecrolimus (contd)
  • 20 out of 23 children investigated had at least
    one detectable blood level as compared to adults
    (13 out of 25 investigated) over a 3 week period.
  • In 22 pediatric patients aged 3 to 23 months with
    10-92 BSA involvement, a higher proportion of
    blood levels ranging from 0.1 to 2.6 ng/ml (LOQ
    0.1 ng/ml) was seen.

9
Pharmacokinetic studies for Pimecrolimus (contd)
  • This increase may be due to larger surface area
    to body mass ratio seen in younger subjects.
  • A higher incidence of upper respiratory
    symptoms/infections was also seen in the 3-23
    months age group relative to the older age group
    in PK studies.
  • A causal relationship between these findings and
    Elidel use cannot be ruled out.

10
Pharmacokinetics (contd)
  • Some factors leading to higher systemic levels
    include
  • Higher body surface area
  • Younger age groups, especially the 3 to 23 month
    age groups as seen with pimecrolimus, this may be
    due to larger surface area to body mass ratio
    (this age group has not had pharmacokinetic
    testing for tacrolimus levels)
  • Reduced skin barrier function eg. Nethertons
    syndrome

11
Pediatric clinical studies
  • Use of Protopic 0.03 ointment was studied in
    children 2-15 years of age by conducting 2 Phase
    3 studies.
  • In these studies, varicella zoster and
    vesiculobullous rash were seen more frequently in
    patients treated with Protopic ointment 0.03,
    compared to vehicle.

12
Pediatric clinical studies (contd)
  • Elidel cream 0.1 was studied in infants 3-23
    months of age and in children 2-17 years of age.
  • In the 2-17 years age group, nasopharyngitis,
    influenza, viral infections, pyrexia ,cough,
    headache, eczema herpeticum were increased over
    vehicle in the 1 year safety study.

13
Pediatric clinical studies (contd)
  • In the 3-23 months short term (6 week) infant
    study, pyrexia, URI, nasopharyngitis,
    gastroenteritis, otitis media, diarrhea seen more
    frequently compared to vehicle. The adverse event
    incidence for those in the open label phase of
    this study who switched over to Elidel cream from
    vehicle approached the incidence of those
    patients who remained on the cream.

14
Pediatric clinical studies (contd)
  • In the 6 month infant study safety data, adverse
    events occurring more frequently in the Elidel
    cream group compared to vehicle included pyrexia,
    URI, cough, vomiting, hypersensitivity, rhinitis,
    viral rash, rhinorrhea, and wheezing.

15
Indications for use (Second-line)
  • Both Protopic and Elidel are indicated for
    patients in whom the use of alternative,
    conventional therapies are deemed inadvisable
    because of potential risks, or in the treatment
    of patients who are not adequately responsive to
    or are intolerant of alternative, conventional
    therapies

16
Proposed Mechanisms of Action
  • Both Tacrolimus and Pimecrolimus inhibit
    T-cell activation by binding to the same
    cellular receptor, the FK-binding protein (FKBP)
    or macrophilin-12.
  • The tacrolimus/pimecrolimus-FKBP complex
    further binds to calcineurin, which is an enzyme
    vital for early activation of both T helper cell
    types 1 and 2.

17
Adverse Effects of Topical Immunosuppressants
  • Local (Application site)
  • Burning
  • Pruritus
  • Erythema
  • Irritation
  • Edema
  • Urticaria

18
Adverse effects of Topical Immunosuppressants
(contd)
  • Systemic
  • Pyrexia
  • Upper and lower respiratory tract infection
  • Nasopharyngitis
  • Viral skin rashes eg. molluscum contagiosum,
    herpes simplex, herpes zoster, eczema herpeticum
  • Influenza

19
Adverse effects of Topical Immunosuppressants
contd
  • Systemic side effects contd
  • Otitis media
  • Gastroenteritis, vomiting, diarrhea
  • Streptococcal pharyngitis, staphylococcal
    infection
  • Skin infection NOS
  • Lymphadenopathy - In absence of a clear etiology
    or in the presence of acute infectious
    mononucleosis, discontinuation recommended. Close
    monitoring required.

20
Adverse effects of Prograf
  • Patients receiving Prograf are at an increased
    risk of developing lymphomas and other
    malignancies, particularly of the skin. The risk
    appears to be related to the intensity and
    duration of immunosuppression. A
    lymphoproliferative disorder (LPD) related to
    Epstein-Barr virus infection has been reported in
    immunosuppressed patients. The risk of LPD
    appears greatest in young children who are at
    risk for primary EBV infection while
    immunosuppressed.

21
Potential long-term adverse effects of topical
immunosuppressants
  • Increased incidence of malignancies in animal
    studies with topical tacrolimus(T) and
    pimecrolimus (P)
  • Lymphomas P T
  • Follicular cell adenomas P
  • Skin tumors (with concurrent UV radiation
    exposure) P T

22
Potential long-term adverse effects (contd)
  • Since systemic use of calcineurin inhibitors
    is associated with formation of lymphomas and
    skin malignancies, low systemic exposure from
    topical calcineurin inhibitors over a course of
    time leading to a cumulative dose effect may lead
    to melanomas, non-melanoma skin cancers,
    Hodgkins and Non-Hodgkins lymphomas

23
Concerns about long term side effects
  • Children from the age of 2 years and upwards
    (with off- label use expected in even younger
    children) will be using these medications on a
    short or intermittent long term basis
  • About one third of children with moderate-severe
    AD may continue to use these drugs into teenage
    and adult years, thereby having a long duration
    of exposure.

24
Concerns about long term side effects (contd)
  • Currently, we do not have long term safety data
    on either Tacrolimus or Pimecrolimus.
  • Postmarketing evaluation of topical
    immunosuppressants is needed to evaluate this
    potential risk. Means of setting up these
    prospective studies need to be discussed.
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