7. General Rheumatology 3 Osteoarthritis (OA), Rheumatoid Arthritis (RA), Adult Still Disease II.pdf

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Steven C Kimmel, MD, FACR, FACP, CTI, RhMSUS
Disclosures
(Grant Research Support)
Roche Novartis
Amgen Anesiva
Genetech Wyeth
Centacor Bionicare
Searle Abbott
GE Lunar Corp Meditrend
Teragenix Pfizer
Immunicon Purdue Pharma LP
UAB Proctor and Gamble
Lilly BMS
 Osteoarthritis
and
Rheumatoid Arthritis
Steven Kimmel, M.D.
West Broward Rheumatology Associates
(American Arthritis and Rheumatology Associates)
 RA: Therapy
Baseline Therapy: Same as for OA
PT
Analgesics
NSAIDs
Injections (steroids / No Hylans )
Surgery
Other Options
Steroids (oral)
cDMARDs: (Conventional DMARDs)
bDMARDs (Biologic DMARDs)
Oral “Biologic” DMARDs:
Protein Kinase inhibitors: JAK Kinase inhibitor
 RA Linear Progression
Early RA Intermediate Late
Inflammation
Radiographs
Severity (Arbitrary Units)

Disability
Late Intervention
Early Intervention

0 5 10 15 20 25 30

Duration of Disease (years)

Graph: Adapted from: Kirwan JR. J Rheumatol. 2001;28:881-886.
Photo: Copyright © American College of Rheumatology.
 RA: Therapy
Biologic
Steroids NSAIDs cDMARDs DMARDs
Oral COX-2 Specific Anti-Malarials Anti TNF
< 20 mg/day or Selective
SQ injection High doses Sulfasalazine Anti T-Cell

IV if needed Low dose as MTX Anti B-Cell
adjunct for pain Leflunomide
Intra-articular Azathioprine Anti IL-6
Cyclosporine
MMF
JAK kinase inh

Disease Will Progress Prevent Disease Progression
Decrease Life Expectancy Improve Life Expectancy
 NSAID Agents
Most commonly prescribed agents
Many available OTC (over the counter)

Provide pain relief in both OA and RA
Do not prevent progression of RA
ADVERSE EVENTS:
– > 10 % dyspepsia
– 1-10 %
Gastric or small bowel bleed / ulceration
Renal insufficiency
– < 1%
CNS confusion
Hepatic / Hematologic / Rash / Respiratory
– ? CARDIOVASCULAR
– GREATEST CAUSE OF DEATH OF ANY MED GROUP

Adapted from American College of Rheumatology Ad Hoc Committee on Clinical Guidelines.
Arthritis Rheum. 1996; 39:723-731.
 RA: Pros and Cons of Steroid Therapy
Pros Cons
Anti-inflammatory
and Doesnot conclusively affect
immunosuppressive effects disease progression
RAPID ONSET so can be Tapering and discontinuation
used to bridge gap between of use often unsuccessful
initiation of DMARD
Even low doses result in skin
therapy and onset of action
thinning, ecchymoses, infections
and Cushingoid appearance
Significant cause of steroid-
induced osteopenia / increase
atherosclerosis
Decrease long term life
expectancy
 RA: Choice of cDMARD
Mild Features Aggressive Features

Sulfasalazine Methotrexate
Avoid if Sulfa Allergy
Leflunomide
Hydroxychloroquine
Avoid if retinal disease Azathioprine
Avoid if low G6PD
DMARDs: Beware the Dark Side
All DMARDs have side effects

HCQ can deposit in the retina after 5
years of use

MTX may cause serious problems
Lung
Liver
Bone Marrow

Be on the look out for toxicity with
all the DMARDs.
RA: Biologic DMARDS
 RA: Available Biologic Agents
TNF Inhibition
Infliximab Chimeric anti-TNF-α mAb Ab to TNF

Etanercept TNF-receptor p75 IgG1 Soluble receptor
Adalimumab IgG1 mAb (humanized) Ab to TNF
Golimumab mAb Ab to TNF
Certolizumab mAb attached to PEG Ab toTNF (Pegylated )

IL Inhibition
Anakinra IL-1 IL-1 Receptor inhib
Tocilizumab IL-6 Ab to IL-6 receptor
Sarilumab IL-6 Ab to IL-6 receptor
Cell Inhibitors
Rituximab B-Cell Inhibitor anti-CD20
Abatacept T-Cell Inhibitor CTLA-4 Ig
Oral Biologic Agents – Protein Kinase inhibitors
Tofacitinib JAK Kinase inhibitor Taken Orally
Baricitinib /
Upadacitinib Red: IV only; Yellow: SQ only; Green: IV or SQ; White: PO
 Biologic Rx: Contraindications
Multiple sclerosis, optic neuritis (no TNF Rx)
H/O Serious or recurrent infections
History of TB or positive PPD test (untreated)
– (Treat or Use t-cell therapy / Abatacept)
Hepatitis B
– (Avoid TNF and B-cell agents, others unclear)
Congestive heart failure
Lymphoma (? wait 5 years after treatment / use Rituximab)
Vaccinations: No Live Virus Vaccines
– (need to wait 4 weeks after live vaccination)
 RA: Current Approach
New Emphasis in Management
Early Diagnosis (using new criteria)

TREAT TO TARGET (using an
objective measure of disease activity):
– Early use of cDMARDs
– Early use of Biologic agents
– Use of multiple cDMARD regimens or
combination cDMARD and Biologic agent
– Appropriate use of steroids

Control Co-Morbid Conditions
 RA: Treat To Target
Clinical Remission:
– Low disease activity with no synovitis

Clinical and Radiographic Remission
– Low disease activity with no synovitis
– No radiographic evidence of ongoing disease (US / MRI)

Immunological Remission
– Low disease activity with no synovitis
– No radiographic evidence of ongoing disease (US / MRI)
– No serologic evidence of disease presence
 RA: Co-Morbid Conditions
Osteoporosis
– RA is an independent risk factor
Cardiovascular Disease
– Heart attacks
– CVA
Vaccinations (current recommendations)
– Killed virus / recombinant vaccines: Should give
Shingrix (once x 2 doses)
Fluviron (yearly)
Pneumovac (every 5 years x 2)
Heptavac (once)
TDap (every 10 years)

– Try to AVOID Live Virus Vaccines: Flumist / Measles / yellow fever
Aim to finish vaccination four weeks prior to Biologic treatment or withhold Biologic treatment for 3
months then vaccinate and wait 4 weeks

– COVID Vaccine – T cell and B cell therapies associated with poor response.
Inject end of interval wait 1 week for next dose
 RA: Prognosis
In the past (pre-biologic era)
Gold Therapy: < 5% remission
Methotrexate: ~ 20 % remission

Currently (Biologic Era):
60% complete remission
90% partial remission

The future (Treat to target) / New agents ?
Possible change in target to serologic remission
Rheumatoid Arthritis: Extra Topics
Extra-articular Disease
Cervical Spine Disease
Adult Onset Stills Disease
Felty’s Syndrome
Women’s Health Issues
Disability
RA: Extra-articular Disease
Rheumatoid Nodules
Ocular involvement
Uveitis
Rheumatoid nodules
Pulmonary Disease
Solitary or multiple nodules:
– do not assume RA rule out CA
Interstitial Lung Disease
Pulmonary HTN
Vasculitis
Cardiac
– Carditis / pericarditis
Neurologic
– Mononeuritis multiplex
Skin
– Vasculitic ulcers
– Amyloidosis
The Rheumatoid Neck: C1-C2
Criteria For The Diagnosis of Adult Still’s Disease
All required for diagnosis:
Fever > 39°C
(Qoutidian: reaching normal once daily)
Arthralgia or Arthritis
Rheumatoid Factor < 1:80
ANA < 1:100

In addition to any two of the following:
White cell count > 15,000 cells/mm3
Still’s rash
Pleuritis
Pericarditis
Hepatomegaly or splenomegaly or
generalized lymphadenopathy

Adapted from Cush et al
Adult Onset Still’s Disease: Rash

Faint salmon-colored rash
Most common on the trunk and upper extremities
May also be seen on the face
 Adult Onset Still’s Disease
Complications
Pericardial Tamponade
Myocarditis
Pneumonitis
Intravascular coagulopathy (DIC)
Increasing LFT / Hepatic Necrosis
Macrophage activation syndrome (HLH)
decreased plt, hgb, HSM
Prognosis:
Poor Prognosis: Shoulders / hips
> 4 joints

After 10 years 1/2 still on DMARDs
1/3 still on steroids
 Adult Onset Still’s Disease
LABS:
Ferritin highly elevated in >70%
Can be used to follow response

COURSE:

Monophasic:
systemic features predominate < 1 year

Intermittent:
intermittent flares of arthritis with remissions

Chronic:
arthritis predominates – can be erosive
 Adult Onset Still’s Disease
Treatment
NSAIDs:
¼ will respond
High doses
Beware abnormal LFTs watch closely
Steroids: - For non-responders
- For those with increased LFTs
- For severe cases
DMARDs: - Hydroxychloroquine
- Increased toxicity Sulfasalazine
- Methotrexate: care with LFTs
Biologic Therapy:
– IL-1 inhibition: Anakinra, Canakinumab
– IL-6 inhibitor: has best data to date – still off label
– TNF inhibitors: can work off label
 Felty’s Syndrome
Seropositive RA
– HLA DR4 95%
– More severe RA manifestations (Vasculitis,
mononeuritis, Nodules, etc)

Granulocytopenia

Splenomegaly
– most patients (90%) but not required

TREATMENT:
– Low Neutrophil Count: GM-CSF
– RA: cDMARD / Biologics
RA: Women’s Health Issues

Contraception
Pregnancy
Lactation
Menopause
Women’s Health Issues: Pregnancy
80% of individuals with autoimmune disease in the US are
women

50% of pregnancies are unplanned so it is important to consider a
woman’s reproductive journey including the potential for
pregnancy in all patients of reproductive age

Its important to maintain control of disease activity and to select
an agent that can be used before, during and after pregnancy.

Ab transfer depends on the presence of the Fc portion and varies
by trimester. No transfer the first trimester but IgG/ biologic
transfer can occur as early as 13 weeks, in the 2nd trimester and
peaks during the 3rd trimester.
 RA: Women’s Health Issues
SAFE
– Hydroxychloroquine
– Certilizumab
Contraception is necessary on and after certain
medicines:
DMARDs
– Cyclophosphamide
– MTX 3-6 months after
– Leflunomide 2 years after
– MMF
– AZA
Biologic DMARDs
– Anti-CD 20
– Anti-IL-6, anti- IL-1, anti-IL12/23, T cell
costimulatory modulators, anti-BAFF
IUD’s ? increased risk for infection
BCP’s possibly improve symptoms in some
 RA: Women’s Health Issues
Vaccination:

– Need to be up to date prior to starting a family

– Live viruses vaccines
need to be given before biologic agents started then wait 4-5
weeks and can start biologic
Can stop biologic wait 3 months then vaccinate then wait 4-
5 weeks and restart
RA: Women’s Health Issues
Pregnancy
Maternal issues: Favorable on
Mother
– 54 % improve
– 46 % either remain stable or worsen,
– but > 90% relapse postpartum

Fetal issues:
– increased risk for fetus from medicines
– Outcomes related to maternal disease
activity
Preterm delivery
Small for gestational age
C-section
RA: Women’s Health Issues
Lactation:

Some meds okay:
– Hydroxychloroquine
– Certilizumab

Others not clear:
– Biologics ? Abs with Fc portion do get into breast milk
Babies with Fc receptors in GI epithelium
Metabolized in GI tract?

Others avoid:
– MTX
– Lef
RA: Women’s Health Issues
Menopause

Increased risk of RA in post-menopausal
women
Coronary risk increased
Coronary risk increased further in those on
steroids
RA is an independent risk factor for the
development of Osteoporosis
Disability: Was this Artist disabled ?
Pierre-Auguste Renoir
1841 - 1919

Rheumatoid
Arthritis
1888 - 1919
Pierre-Auguste Renoir
1841 - 1919

Rheumatoid
Arthritis
1888 - 1919
 Case 1
A 68 year old female patient c/o difficulty closing
her fingers that has progressed over many years.

Case 2
A 45 year old white female presents for evaluation
of swelling in her fingers and wrists that has been
present for 4 weeks.
 OA / RA Cases
How do we tell which patient
has OA and which has RA?
1. History and Physical
2. Labs
3. X-rays
4. scans
 Case 1 Hx Case 2 Hx
A 68 year old female patient c/o A 45 year old white female
difficulty closing her fingers that presents for evaluation of
has progressed over many years. swelling in her fingers and wrists
that has been present for four
weeks.

She denies morning stiffness or She denied any fevers or rashes.
redness in the fingers but notes She also noted shoulder and knee
they are knobby and was told pains as well as swelling more
that she could have RA by her recently. She has stiffness in the
daughter who is a nurse so she morning lasting for two hours
and improving faster with a hot
comes to you for your opinion.
shower.
 OA / RA Cases: Hx
Patient 1 Patient 2
68 yo 45 yo
Fingers / wrists/
Fingers
shoulders/ Knees
Sx with use Better with use
No stiffness in am AM Stiffness
 Case 1 PE
Her physical exam revealed a normal general exam. Extremities with
fingers showing DIP and PIP ony changes. Hips with mild decreased
internal and external rotation. Knees, ankles and feet were normal.
Her legs had no clubbing cyanosis or edema.
 Case 2 PE
Her exam revealed finger swelling as shown in the next slide
bilaterally with synovitis and tenderness in the 2-4th PIP and 1,2,3rd
and 5th MCP joints. Her wrists had flexion / extension of 60
degrees with mild synovitis and pain on palpation. Shoulders had
slightly decreased active range of motion and passive range of
motion and were tender to touch. Her knees had full range of
motion but mild warmth and effusions bilaterally with tenderness to
palpation. Her elbows, hips, ankles and feet were normal.
 OA / RA Cases: PE
Patient 1 Patient 2
Finger swelling (Boney) Finger swelling (Boggy)

DIP and PIP MCP and Wrists

No redness or warmth Red / Warm

No other swollen joints Other joints: Shoulders /
Knees
 Cases LABS
What labs are needed to tell which of these is OA or RA?
a. ANA and RF
b. ESR and C-RP
c. RF and ACA
d. All of the above
e. None of the above

Which labs do you want to check to determine how to treat these patients ?
a. CBC
b. Chemistries
c. LFT
d. U/A
e. All of the above
 Putting It All Together
MONOARTHRITIS ACUTE Trauma ? Yes – X Ray
No - ?inflammation

Inflammation ? YES – Aspirate
No - TP’s ?

CHRONIC Inflammation ? Yes – Aspirate / Bx
No - TP’s ?

POLYARTHRITIS Synovitis? No TP? Bursitis /Tendonitis
CASE 1 STS: Hard /bony
Firm /nodular
YES ACUTE Asymm DGI, Staph, Lyme, Early SpdA /CTD
Symm Viral, SBE, ARF, GC, CTD

CHRONIC Asymm SpdA, Cryst, CTD, Atyp RA
CASE 2 Symm CTD (see labs)
 Case 1
Irrelevant of labs, which of the following treatments
should be avoided in the first patient but started as soon
as possible in the second patient?

a. NSAIDs
b. Acetaminophen
c. Tramadol
d. DMARD therapy
e. Steroid injections
 Case 2
45 year old white female swelling
in her fingers and wrists stiffness in
the morning for two hours for 4
weeks

Synovitis on exam – multiple joints

Her joint count is: 18 Swollen
20 Tender

Site Hands Wrists Elbows Shoulders Knees Totals
Swollen 14 2 0 0 2 18
Tender 14 2 0 2 2 20
 Case 2
Her labs revealed: Her Serologies reveal:
CBC: WBC= 6.2
Hgb = 10.5 ESR = 95 (nl < 20)
Plt = 185 K C-RP = 15 (nl < 1)
MCV = 90
RDW = 12 RF = 28 (nl < 14)
SMA7: Cr = 1.0 ACPA = > 250
LFT: nl ANA = negative
TFT: nl

X-rays of her hands and
wrists are normal.

DOES she have RA based on the:
1987 Criteria ?
2010 Criteria ?
 Case 2
1987 Criteria:
Criteria she has: Criteria she does not have:
hand and wrist involvement X-ray changes
Symmetric pattern Rheumatoid Nodules
>3 joints
Am Stiffness
RF * SYMPTOMS MUST BE PRESENT FOR 6 WEEKS TO COUNT

2010 Criteria

DOMAIN POINTS
Joint Involvement 5
Serology 3
Acute Phase Reactants 1
Duration (>6 weeks) 0

Total 9
 2010 ACR Criteria for RA:
1) have at least 1 joint with definite clinical synovitis (swelling)
2) with the synovitis not better explained by another disease
(fulfill criteria if score of A-D is ≥ 6/10)
A Joint Involvement Score
1 large joint 0
2 – 10 large joints 1
1 – 3 small joints (with or without large joint) 2
4 – 10 small joints (with or without large joint) 3
> 10 joints (at least 1 small joint) 5
B Serology (at least 1 test result is needed for classification)
Negative RF and negative ACPA 0
Low-positive RF or low-positive ACPA 2
High-positive RF or high-positive ACPA 3
C Acute-phase reactants (at least 1 test result is needed)
Normal CRP and normal ESR 0
Abnormal CRP or abnormal ESR 1
D Duration of symptoms
< 6 weeks 0
> 6 weeks 1
What if the ANA was Positive?

Does she have RA?

Does she have SLE?
 Interpretation of a Positive ANA

Actual Ratio
RA:SLE = 40:1
80%RF

95% ANA 20% ANA

30%RF

Patients with SLE Patients with RA
 Evaluation of the patient with
Symmetric Polyarthritis > 6 weeks
Rheumatoid Factor
+ -
ANA ANA
+ - + -

RA, SLE or Strong evidence SLE or other Strong evidence
against SLE against SLE
other CVD CVD
Seroneg RA,
Possible RA or other Spondylo-
Check other immune stimulatory RA unlikely arthropathy or other
Autoantibody disease immune complex
studies Check other disease (SBE, Cryo)

Autoantibody
studies
Osteoarthritis Rheumatoid Arthritis

A degenerative disease An inflammatory disease
involving primarily of unknown etiology.
cartilage.

The most common form There is an increased
of arthritis. mortality associated with
this disease.

Treatment is aimed at Treatment is aimed at
pain control and controlling disease activity
improvement / hopefully slowing the joint
preservation of function. damage, alleviating pain and
maintaining function.

Surgery is reserved for those with severe disease symptoms
unresponsive to medical therapy.