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 Present at seminars sponsored by the following pharmaceutical companies:
 Biogen-Idec
 EMD-Serono
 QuestCor
 Teva Neurosciences
 Engage in research for the following companies:
 Biogen-Idec
 Elan
 EMD-Serono
 Janssen
 Pfizer
 Roche
 Teva Neurosciences
 A disorder or group of disorders affecting the CNS -
central nervous system (brain, spinal cord)
 An autoimmune process causing inflammation in the
CNS in genetically susceptible individuals after one or
more triggers
 Inflammation involves myelin, causing demyelination
in the CNS, which leads to slower nerve conduction
and reduced nerve signals controlling function
 Axonal injury and destruction occur early and are
associated with permanent neurological dysfunction
Joints: Rheumatoid Arthritis, Lupus, Psoriatic arthritis
Muscles: Polymyositis; Neuromuscular junction: Myasthenia Gravis
Peripheral Nerves: Guillain Barré, CIDP
Skin: Psoriasis, Dermatomyositis, Lupus
Blood Vessels: Lupus, Polyarteritis Nodosa, Temporal Arteritis
Blood: TTP (platelet disorder)
Sinuses: Allergic Rhinitis
Thyroid: Thyroiditis
Lungs: Asthma
Gastrointestinal: Crohn’s Disease, Autoimmune Hepatitis, UC
Kidney: Glomerulonephritis
Pancreas: Juvenile Diabetes
 Infection
 Lyme disease
 Neurosyphilis
 PML, HIV, HTLV-1
 Inflammatory
 SLE
 Sjögren’s
 Other CNS vasculitis
 Sarcoidosis
 Behçet’s disease
 Guillain Barré
 Myasthenia Gravis
 NPH
 Trauma (chronic SDH)
 Vascular
 Multi-infarct state
 Metabolic
 Vitamin B12 and E
deficiencies
 Thyroid disorders
 CADASIL - rare/familial
 Cancer
 CNS lymphoma
 Paraneoplastic syndrome
 Congenital
 Chiari malformation
 Syringomyelia
 Degenerative
 Cervical spondylosis
 Motor neuron disease (ALS
and SMA)
1. Relapsing-remitting 2. Primary-progressive
3. Secondary-progressive 4. Progressive-relapsing
Time Time
Time Time
Increasingdisability
Increasingdisability
Increasingdisability
Increasingdisability
Adapted from: Lublin FD, Reingold SC. Neurology. 1996;46:907-911.
5-10%
66%
of
RRMS
5-10%
80-85%
 Relapses
 Focal disturbances of function >24 hours
 Follows stability of at least 30 days
 In absence of environmental, metabolic, or infectious
processes
 Occur on average once a year in untreated patients (highly
variable)
 Over time, frequency of relapses typically drops, even w/o
treatment (so any treatment looks favorable if not
compared with placebo or other standard DMT’s)
 Prevent Relapses
 Treat Relapses
 Learn to recognize mimics / pseudoexacerbations
 Manage symptoms – acutely during relapses and
chronically if they persist
 Delay progression to disability (DMT)
 Stabilizing or improving the MRI
 Non-Medical Management:
 Rest in a cool environment
 Symptomatic - treatment of individual symptoms:
 Cognition
 Fatigue
 Muscle spasms / stiffness
 Nerve pain / neuralgia
 Ataxia
 Bladder difficulties
 Seizures
 Medical Management:
 IV Therapy:
- methylprednisolone, 500-2000 mg IV for 3-5 days, sometimes
followed by a short course of prednisone over 1-3 weeks; MOA =
cortisol effect on inflammation, stabilizing the BBB
- Acthar gel, IM/SC, 80-120 units daily for 5-21 days (when IV
steroids are poorly tolerated or ineffective or if the patient has
poor IV access) – comparable in benefit and side effects, but
different MOA = cortisol + melanocortin effects (may have
advantages over steroids, with loss cortisol effects and more
immune cell effects in the brain and throughout the body)
 Oral steroids:
- prednisone, methylprednisolone, or dexamethasone
- high doses are more effective and reasonably well tolerated
- used for people with poor IV access or can’t tolerate IV steroids
 Other Therapy: plasmaphoresis, IVIg, cyclophosphamide
 Diet: NMSS website. Also: The Zone Diet, by Dr. Barry Sears, hunter-gatherer
variation by Dr. Terry Wahls:
http://www.youtube.com/watch?v=KLjgBLwH3Wc&feature=youtube_gdata_player
 Vitamin D3 supplementation
 Exercise: stretching, weight training, aerobic conditioning; keep in the best
shape possible to be able to fight against any future challenges / attacks
 Sleep: quality and quantity
 Rest: planned rest periods for energy conservation
 Others: relaxation exercises, biofeedback, meditation, tai chi, yoga
 Foreign Substances:
 eliminate tobacco use
 alcohol (ok in small amounts - 1-2 beverages per day)
 marijuana (probably ok in small amounts)
 medications, especially sedatives, in combination with the above
Be aware of conditions or factors that may mimic or aggravate MS symptoms
 stress, depression, sleep deprivation, medical conditions (UTI,
bronchitis/lung disorders, thyroid disorders, heart disease), and effects of
medications
 Educate yourself on all available treatments
 Adjust the intensity of treatment to the severity of disease (risk
vs. benefit)
 Be realistic about what treatments can offer – they don’t cure
MS and may only keep you from declining
 Treat early, stay positive, and stay committed to your chosen
therapy.
 Don’t be afraid to change therapies if the current one isn’t right
for you (intolerable side effects or not providing benefit); on the
other hand, think twice about going off a therapy that is
working
 Be open and honest with your family, physician, and most of
all, yourself
 “MS is a marathon, not a sprint. It’s not how you start, but how
you finish that’s important.”
- Dr. Randall Schapiro
Natural course of disease
Theoretical Model
Later intervention
Later
treatment
Treatment
at diagnosis
Intervention at diagnosis
Time
Disease onset
Disability
Currently not submittedFDA-approved therapies
1995 2000 2005 2009 2010 2011
Alemtuzumab
Extavia®
(IFNβ-1b)
Gilenya™
(fingolimod)
Tysabri®
(natalizumab)
Betaseron®
(IFNβ-1b)
COPAXONE®
(glatiramer acetate injection)
Avonex®
(IFNβ-1a)
Rebif ®
(IFNβ-1a)
Novantrone®
(mitoxantrone)
Laquinimod
Approval date
2012 2013
Aubagio
(teriflunomide)
Daclizumab
Tecfidera
(DMF/BG12)
1
8
Lymph node
Bloodstream
Naïve T cells
Anti-inflammatory Th2 cells (MS-specific)
• Multiple sclerosis is a
debilitating autoimmune
disease characterized by
both inflammation and
axonal degeneration1
• In order to regulate CNS
damage, treatment of MS is
focused on restoring
immune system balance2-5
• It is important to expand our
view to consider treatment
impact on the overall
immune response
1. Kasper LH, et al. Neurology. 2010;74(Suppl1):S2-S8. 2. Ziemssen T. J Neurol. 2005;252(Suppl 5):V/38-V/45. 3. Yong VW, et al. Neurology. 2007;
68(22 Suppl 3):S32-S37. 4. Dhib-Jalbut S. Neurology. 2007;68(22 Suppl 3):S13-S21. 5. Tzartos JS, et al. Am J Pathol. 2008;172(1):146-155.
Proinflammatory Th1 cells (MS-specific)
1
9
MS-specific proinflammatory
immune cells cross from the
bloodstream into the central
nervous system (CNS),
secrete proinflammatory
cytokines, and eventually
destroy myelin and facilitate
neuronal death.
1. Ziemssen T. J Neurol. 2005;252(Suppl 5):V/38-V/45. 2. Yong VW, et al. Neurology. 2007;68(22 Suppl 3):S32-S37. 3. Dhib-Jalbut S. Neurology.
2007;68(22 Suppl 3):S13-S21. 4. Tzartos JS, et al. Am J Pathol. 2008;172(1):146-155.
Proinflammatory cytokinesProinflammatory Th1 cells (MS-specific)
Proinflammatory cells
release destructive cytokines
and neurotoxic agents
Blood-brain barrier
Th1 cell crossing
blood-brain barrier
Normal MS
Inflammatory
IFN-
IL-12
TNF
Inflammatory
IFN-
IL-12
TNF
Anti-inflammatory
IL-4
IL-10
TGF-
Anti-inflammatory
IL-4
IL-10
TGF-
Step 1: Main (Platform) medications
 Interferon beta (Avonex, Rebif, Betaseron, Extavia)
 Glatiramer acetate (Copaxone)
 Natalizumab (Tysabri)
 Fingolimod (Gilenya)
 Teriflunomide (Aubagio)
 Dimethyl Fumarate (Tecfidera)
Step 2: Switch between the platform agents if an agent is
ineffective (based on several factors) or poorly tolerated
Step 3: Add IV methylprednisolone or IM/SC ACTHAR (short
course vs. pulses); pulse therapy is not permitted in
combination with Tysabri
Step 4: Switch to or add (except Tysabri) immunosuppressants
 Imuran, CellCept -> methotrexate -> cyclophosphamide or mitoxanthrone
Other alternatives: Experimental agents prior to release onto
the market; some protocols contain a placebo arm; relapsing
and progressive MS (Melbourne, Vero Beach, Orlando,
Maitland)
Future oral agents (daily) - laquinimod (2013/2014)
Infusions – alemtuzumab (IV yearly), rituxumab / ocrelizumab
(IV every 6 months)
Injections: daclizumab (IM every 2 weeks)
Stem cells – currently limited to RRMS
Bone marrow transplantation
Implanting stem cell and other immature cells, such as
oligodendrocyte progenitor cells in brain / spinal fluid
Closely monitor disease activity and response to therapy
 Careful history of relapses, progression, and side effects of medications
 Neurological examination
 MSFC (Multiple Sclerosis Functional Composite: Timed 25ft Walk, 9-
hole peg test, PASAT)
 EDSS (Expanded Disability Status Score): cognitive, visual, brainstem,
motor, cerebellar, sensory, bowel/bladder
 Neuropsychological testing (Cognitive/Emotional)
 MRI’s of the brain and upper (C-/T-) spine
 Evoked potentials
 OCT / V.A. (especially with varying contrasts) / Visual Field testing
 Blood work (25-hydroxy-vitamin D levels, CBC/LFT’s)
 Quality of Life
The New Yorker www.cartoonbank.com
 The ability to follow the treatment plan
that you and your health care
provider agreed upon (a contract)
 Average adherence = 50%
 Factors interfering with adherence:
 treatment (especially needle) fatigue
 loss of motivation / complacency
 financial challenges
 lack of curative benefit
 unrealistic expectations (of cure, reversal of
disability, resolution of current symptoms)
 adverse effects of medications
 pregnancy
 doctor recommended against it
 treatment was “a hassle”
 Patients who stopped DMTs had:
 more severe disability, including SPMS
 more relapses
 poor to fair health
 depressed mood
 Reasons for never using DMT:
 my MS was not severe enough
 doctor didn’t recommend it or advised against it
 fear of DMT making things worse of causing
adverse effects
 cost
 used other therapies
 fear of needles
 didn’t know about the DMTs
 Improving adherence:
 encouragement
 education, especially importance of treatment
 manage medication side effects
 injection technique and follow-up
 work with emotional issues (anxiety and
depression)
 recognize and work around cognitive deficits
 integrate a treatment schedule into the patient’s
lifestyle
 encourage a team approach – patient, family,
friends, nurses, clinicians, self-help groups, and
pharmaceutical support programs
 Determine what’s most important in your life - prioritize
based on your limitations at any given time
 Keep active with family and friends
 Be active in your church, synagogue, and community
 Improve your lifestyle - exercise regularly, do yoga and tai
chi, eat a balanced diet, with small amounts through the
day, avoid tobacco, avoid excessive alcohol
 Look at the “big picture” – don’t sweat the small stuff
 Don’t dwell on the things you can’t change; focus on what’s
truly important…
Thank You
for
Your Attention!

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Advancements In Treatment Options MS Relapses & Adherence

  • 1.
  • 2.  Present at seminars sponsored by the following pharmaceutical companies:  Biogen-Idec  EMD-Serono  QuestCor  Teva Neurosciences  Engage in research for the following companies:  Biogen-Idec  Elan  EMD-Serono  Janssen  Pfizer  Roche  Teva Neurosciences
  • 3.  A disorder or group of disorders affecting the CNS - central nervous system (brain, spinal cord)  An autoimmune process causing inflammation in the CNS in genetically susceptible individuals after one or more triggers  Inflammation involves myelin, causing demyelination in the CNS, which leads to slower nerve conduction and reduced nerve signals controlling function  Axonal injury and destruction occur early and are associated with permanent neurological dysfunction
  • 4. Joints: Rheumatoid Arthritis, Lupus, Psoriatic arthritis Muscles: Polymyositis; Neuromuscular junction: Myasthenia Gravis Peripheral Nerves: Guillain Barré, CIDP Skin: Psoriasis, Dermatomyositis, Lupus Blood Vessels: Lupus, Polyarteritis Nodosa, Temporal Arteritis Blood: TTP (platelet disorder) Sinuses: Allergic Rhinitis Thyroid: Thyroiditis Lungs: Asthma Gastrointestinal: Crohn’s Disease, Autoimmune Hepatitis, UC Kidney: Glomerulonephritis Pancreas: Juvenile Diabetes
  • 5.
  • 6.
  • 7.  Infection  Lyme disease  Neurosyphilis  PML, HIV, HTLV-1  Inflammatory  SLE  Sjögren’s  Other CNS vasculitis  Sarcoidosis  Behçet’s disease  Guillain Barré  Myasthenia Gravis  NPH  Trauma (chronic SDH)  Vascular  Multi-infarct state  Metabolic  Vitamin B12 and E deficiencies  Thyroid disorders  CADASIL - rare/familial  Cancer  CNS lymphoma  Paraneoplastic syndrome  Congenital  Chiari malformation  Syringomyelia  Degenerative  Cervical spondylosis  Motor neuron disease (ALS and SMA)
  • 8. 1. Relapsing-remitting 2. Primary-progressive 3. Secondary-progressive 4. Progressive-relapsing Time Time Time Time Increasingdisability Increasingdisability Increasingdisability Increasingdisability Adapted from: Lublin FD, Reingold SC. Neurology. 1996;46:907-911. 5-10% 66% of RRMS 5-10% 80-85%
  • 9.  Relapses  Focal disturbances of function >24 hours  Follows stability of at least 30 days  In absence of environmental, metabolic, or infectious processes  Occur on average once a year in untreated patients (highly variable)  Over time, frequency of relapses typically drops, even w/o treatment (so any treatment looks favorable if not compared with placebo or other standard DMT’s)
  • 10.  Prevent Relapses  Treat Relapses  Learn to recognize mimics / pseudoexacerbations  Manage symptoms – acutely during relapses and chronically if they persist  Delay progression to disability (DMT)  Stabilizing or improving the MRI
  • 11.  Non-Medical Management:  Rest in a cool environment  Symptomatic - treatment of individual symptoms:  Cognition  Fatigue  Muscle spasms / stiffness  Nerve pain / neuralgia  Ataxia  Bladder difficulties  Seizures
  • 12.  Medical Management:  IV Therapy: - methylprednisolone, 500-2000 mg IV for 3-5 days, sometimes followed by a short course of prednisone over 1-3 weeks; MOA = cortisol effect on inflammation, stabilizing the BBB - Acthar gel, IM/SC, 80-120 units daily for 5-21 days (when IV steroids are poorly tolerated or ineffective or if the patient has poor IV access) – comparable in benefit and side effects, but different MOA = cortisol + melanocortin effects (may have advantages over steroids, with loss cortisol effects and more immune cell effects in the brain and throughout the body)  Oral steroids: - prednisone, methylprednisolone, or dexamethasone - high doses are more effective and reasonably well tolerated - used for people with poor IV access or can’t tolerate IV steroids  Other Therapy: plasmaphoresis, IVIg, cyclophosphamide
  • 13.  Diet: NMSS website. Also: The Zone Diet, by Dr. Barry Sears, hunter-gatherer variation by Dr. Terry Wahls: http://www.youtube.com/watch?v=KLjgBLwH3Wc&feature=youtube_gdata_player  Vitamin D3 supplementation  Exercise: stretching, weight training, aerobic conditioning; keep in the best shape possible to be able to fight against any future challenges / attacks  Sleep: quality and quantity  Rest: planned rest periods for energy conservation  Others: relaxation exercises, biofeedback, meditation, tai chi, yoga  Foreign Substances:  eliminate tobacco use  alcohol (ok in small amounts - 1-2 beverages per day)  marijuana (probably ok in small amounts)  medications, especially sedatives, in combination with the above Be aware of conditions or factors that may mimic or aggravate MS symptoms  stress, depression, sleep deprivation, medical conditions (UTI, bronchitis/lung disorders, thyroid disorders, heart disease), and effects of medications
  • 14.  Educate yourself on all available treatments  Adjust the intensity of treatment to the severity of disease (risk vs. benefit)  Be realistic about what treatments can offer – they don’t cure MS and may only keep you from declining  Treat early, stay positive, and stay committed to your chosen therapy.  Don’t be afraid to change therapies if the current one isn’t right for you (intolerable side effects or not providing benefit); on the other hand, think twice about going off a therapy that is working  Be open and honest with your family, physician, and most of all, yourself  “MS is a marathon, not a sprint. It’s not how you start, but how you finish that’s important.” - Dr. Randall Schapiro
  • 15. Natural course of disease Theoretical Model Later intervention Later treatment Treatment at diagnosis Intervention at diagnosis Time Disease onset Disability
  • 16.
  • 17. Currently not submittedFDA-approved therapies 1995 2000 2005 2009 2010 2011 Alemtuzumab Extavia® (IFNβ-1b) Gilenya™ (fingolimod) Tysabri® (natalizumab) Betaseron® (IFNβ-1b) COPAXONE® (glatiramer acetate injection) Avonex® (IFNβ-1a) Rebif ® (IFNβ-1a) Novantrone® (mitoxantrone) Laquinimod Approval date 2012 2013 Aubagio (teriflunomide) Daclizumab Tecfidera (DMF/BG12)
  • 18. 1 8 Lymph node Bloodstream Naïve T cells Anti-inflammatory Th2 cells (MS-specific) • Multiple sclerosis is a debilitating autoimmune disease characterized by both inflammation and axonal degeneration1 • In order to regulate CNS damage, treatment of MS is focused on restoring immune system balance2-5 • It is important to expand our view to consider treatment impact on the overall immune response 1. Kasper LH, et al. Neurology. 2010;74(Suppl1):S2-S8. 2. Ziemssen T. J Neurol. 2005;252(Suppl 5):V/38-V/45. 3. Yong VW, et al. Neurology. 2007; 68(22 Suppl 3):S32-S37. 4. Dhib-Jalbut S. Neurology. 2007;68(22 Suppl 3):S13-S21. 5. Tzartos JS, et al. Am J Pathol. 2008;172(1):146-155. Proinflammatory Th1 cells (MS-specific)
  • 19. 1 9 MS-specific proinflammatory immune cells cross from the bloodstream into the central nervous system (CNS), secrete proinflammatory cytokines, and eventually destroy myelin and facilitate neuronal death. 1. Ziemssen T. J Neurol. 2005;252(Suppl 5):V/38-V/45. 2. Yong VW, et al. Neurology. 2007;68(22 Suppl 3):S32-S37. 3. Dhib-Jalbut S. Neurology. 2007;68(22 Suppl 3):S13-S21. 4. Tzartos JS, et al. Am J Pathol. 2008;172(1):146-155. Proinflammatory cytokinesProinflammatory Th1 cells (MS-specific) Proinflammatory cells release destructive cytokines and neurotoxic agents Blood-brain barrier Th1 cell crossing blood-brain barrier
  • 21. Step 1: Main (Platform) medications  Interferon beta (Avonex, Rebif, Betaseron, Extavia)  Glatiramer acetate (Copaxone)  Natalizumab (Tysabri)  Fingolimod (Gilenya)  Teriflunomide (Aubagio)  Dimethyl Fumarate (Tecfidera) Step 2: Switch between the platform agents if an agent is ineffective (based on several factors) or poorly tolerated Step 3: Add IV methylprednisolone or IM/SC ACTHAR (short course vs. pulses); pulse therapy is not permitted in combination with Tysabri Step 4: Switch to or add (except Tysabri) immunosuppressants  Imuran, CellCept -> methotrexate -> cyclophosphamide or mitoxanthrone
  • 22. Other alternatives: Experimental agents prior to release onto the market; some protocols contain a placebo arm; relapsing and progressive MS (Melbourne, Vero Beach, Orlando, Maitland) Future oral agents (daily) - laquinimod (2013/2014) Infusions – alemtuzumab (IV yearly), rituxumab / ocrelizumab (IV every 6 months) Injections: daclizumab (IM every 2 weeks) Stem cells – currently limited to RRMS Bone marrow transplantation Implanting stem cell and other immature cells, such as oligodendrocyte progenitor cells in brain / spinal fluid
  • 23. Closely monitor disease activity and response to therapy  Careful history of relapses, progression, and side effects of medications  Neurological examination  MSFC (Multiple Sclerosis Functional Composite: Timed 25ft Walk, 9- hole peg test, PASAT)  EDSS (Expanded Disability Status Score): cognitive, visual, brainstem, motor, cerebellar, sensory, bowel/bladder  Neuropsychological testing (Cognitive/Emotional)  MRI’s of the brain and upper (C-/T-) spine  Evoked potentials  OCT / V.A. (especially with varying contrasts) / Visual Field testing  Blood work (25-hydroxy-vitamin D levels, CBC/LFT’s)  Quality of Life
  • 24. The New Yorker www.cartoonbank.com
  • 25.  The ability to follow the treatment plan that you and your health care provider agreed upon (a contract)  Average adherence = 50%
  • 26.  Factors interfering with adherence:  treatment (especially needle) fatigue  loss of motivation / complacency  financial challenges  lack of curative benefit  unrealistic expectations (of cure, reversal of disability, resolution of current symptoms)  adverse effects of medications  pregnancy  doctor recommended against it  treatment was “a hassle”
  • 27.  Patients who stopped DMTs had:  more severe disability, including SPMS  more relapses  poor to fair health  depressed mood
  • 28.  Reasons for never using DMT:  my MS was not severe enough  doctor didn’t recommend it or advised against it  fear of DMT making things worse of causing adverse effects  cost  used other therapies  fear of needles  didn’t know about the DMTs
  • 29.  Improving adherence:  encouragement  education, especially importance of treatment  manage medication side effects  injection technique and follow-up  work with emotional issues (anxiety and depression)  recognize and work around cognitive deficits  integrate a treatment schedule into the patient’s lifestyle  encourage a team approach – patient, family, friends, nurses, clinicians, self-help groups, and pharmaceutical support programs
  • 30.  Determine what’s most important in your life - prioritize based on your limitations at any given time  Keep active with family and friends  Be active in your church, synagogue, and community  Improve your lifestyle - exercise regularly, do yoga and tai chi, eat a balanced diet, with small amounts through the day, avoid tobacco, avoid excessive alcohol  Look at the “big picture” – don’t sweat the small stuff  Don’t dwell on the things you can’t change; focus on what’s truly important…