Rheumatoid Arthritis in Pakistan: Symptoms, Causes & Treatment | aihealz
RheumatologymoderateICD-10 · M06.9
Rheumatoid Arthritis.Care & specialists in Pakistan
In Pakistan, rheumatoid Arthritis is managed by rheumatologists. Rheumatoid arthritis is a chronic, symmetric autoimmune polyarthritis in which the body's own immune system targets the synovial lining of joints, producing persistent inflammation, cartilage erosion, and progressive bone damage. It affects roughly 0.5-1% of adults worldwide — about 18 million people in the GBD 2019 estimate — with women diagnosed 2-3 times more often than men and peak onset between ages 40 and 60.
Rheumatoid arthritis (ICD-10: M05 seropositive, M06 seronegative) is a systemic autoimmune disease defined by chronic inflammatory synovitis that, left untreated, erodes cartilage and bone and produces irreversible joint deformity. The disease begins with breakdown of immune tolerance to citrullinated self-proteins; autoantibodies such as rheumatoid factor (RF) and anti-cyclic citrullinated peptide (anti-CCP) antibodies appear in serum years before joint symptoms in many patients. Activated synovial fibroblasts, macrophages, and T and B lymphocytes drive a self-sustaining inflammatory loop dominated by tumor necrosis factor (TNF), interleukin-6 (IL-6), and JAK-STAT signaling. The synovium thickens into a pannus that invades cartilage and subchondral bone, producing the characteristic radiographic erosions.
key facts
Prevalence
0.5-1% of adults globally; 1.3 million US adults (CDC) and ~18 million worldwide (GBD 2019)
Demographics
Women affected 2-3x more often than men; lifetime risk roughly 3.6% women vs 1.7% men
Avg. age
Peak onset age 40-60; can occur at any age including elderly-onset RA after age 65
Global cases
~18 million people worldwide (GBD 2019); incidence rising in older age groups
Specialist
Rheumatology
ICD-10
M06.9
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How you might notice it
The key symptoms of Rheumatoid Arthritis are: Morning stiffness lasting more than 60 minutes that eases with activity through the day — a hallmark distinguishing RA from mechanical joint pain., Symmetric pain, swelling, and tenderness in the small joints of both hands and feet, particularly the metacarpophalangeal (MCP), proximal interphalangeal (PIP), and metatarsophalangeal (MTP) joints, with the distal interphalangeal (DIP) joints characteristically spared., Boggy soft-tissue swelling and warmth over involved joints, distinct from the bony enlargement of osteoarthritis., Persistent fatigue out of proportion to activity, often present months before joint pain becomes evident, and a leading patient-reported symptom in surveys., Low-grade fevers, weight loss, and malaise during active flares, reflecting the systemic inflammatory nature of the disease., Wrist pain and swelling with reduced grip strength — wrist involvement is present in over 75% of patients within the first two years., Foot pain on first weight-bearing in the morning from MTP synovitis; many patients describe walking on pebbles..
01Morning stiffness lasting more than 60 minutes that eases with activity through the day — a hallmark distinguishing RA from mechanical joint pain.
02Symmetric pain, swelling, and tenderness in the small joints of both hands and feet, particularly the metacarpophalangeal (MCP), proximal interphalangeal (PIP), and metatarsophalangeal (MTP) joints, with the distal interphalangeal (DIP) joints characteristically spared.
03Boggy soft-tissue swelling and warmth over involved joints, distinct from the bony enlargement of osteoarthritis.
04
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How it’s diagnosed
diagnosis
Diagnosis of rheumatoid arthritis combines a careful history of inflammatory joint pain, a tender and swollen joint count on examination, serology, acute-phase reactants, and increasingly imaging. The 2010 ACR/EULAR classification criteria (Aletaha 2010) score four domains — joint involvement, serology (RF and anti-CCP), acute-phase reactants (ESR or CRP), and symptom duration of at least six weeks — with a total of six or more out of ten points classifying the patient as having definite RA. The criteria deliberately favor early detection so disease-modifying therapy can start within the so-called window of opportunity in the first three to six months. Rheumatoid factor is positive in roughly 70-80% of patients but is not specific — it occurs in healthy elderly people, hepatitis C, and other autoimmune diseases. Anti-CCP antibodies are present in roughly 70% of patients and carry around 95% specificity, making a positive anti-CCP highly suggestive of RA and an indicator of erosive disease. ESR and CRP are elevated in active disease and used both for diagnosis and for monitoring. Plain radiographs of hands and feet establish baseline and detect periarticular osteopenia or early erosions; magnetic resonance imaging and high-resolution musculoskeletal ultrasound are more sensitive and can show subclinical synovitis and bone marrow edema before erosions appear on X-ray. Synovial fluid analysis is used selectively to exclude crystal arthritis or septic arthritis. The decisive step in practice is referral to a rheumatologist within six weeks of persistent inflammatory joint symptoms — earlier referral and treatment correlates strongly with sustained remission.
Key tests
01
Rheumatoid factor (RF)An IgM antibody directed at the Fc portion of IgG. Present in 70-80% of RA patients but not specific — high titers raise diagnostic confidence and predict more aggressive disease.
02
Anti-cyclic citrullinated peptide (anti-CCP) antibodyHighly specific for RA (~95%) and detectable in early disease, often years before symptoms. A positive anti-CCP predicts erosive, more aggressive disease and shapes treatment intensity.
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Treatment & cost
medical treatments
✓Methotrexate (start 7.5-15 mg orally or subcutaneously weekly; titrate to 25 mg weekly with folic acid 5 mg weekly)
✓Sulfasalazine (start 500 mg twice daily; titrate to 1000 mg twice or three times daily)
✓Leflunomide (loading 100 mg daily for 3 days, then 10-20 mg daily)
surgical options
Synovectomy (open or arthroscopic)Symptomatic relief in 60-80% of selected patients; durability depends on systemic disease control.
Joint replacement arthroplasty — knee, hip, shoulder, MCP10-year prosthesis survival above 90% for total knee and hip arthroplasty; outcomes comparable to osteoarthritis when disease activity is controlled.
Tendon repair and reconstructionRestoration of useful function in roughly 80% of cases when performed within months of rupture.
Cervical spine fusion for atlantoaxial subluxationNeurologic stabilization in over 80% of carefully selected patients; surgery is technically demanding and best done at high-volume centers.
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Causes & risk factors
known causes
Loss of immune tolerance to citrullinated self-proteins
The central pathogenic event in seropositive RA. Peptidylarginine deiminase enzymes convert arginine residues to citrulline; in genetically susceptible people the immune system stops tolerating these modified proteins and generates anti-CCP antibodies that drive synovitis.
Genetic susceptibility, especially HLA-DRB1 shared epitope
Variants in the HLA-DRB1 gene encoding the shared epitope confer a 3-5 fold risk increase and predict seropositive, erosive disease. Other risk alleles include PTPN22, STAT4, and TRAF1-C5; heritability estimates approach 60% for anti-CCP positive RA.
Cigarette smoking
The strongest modifiable risk factor. Smoking promotes lung citrullination of proteins and synergizes with HLA-DRB1 shared epitope to raise anti-CCP positive RA risk up to 20-fold in heavy smokers carrying two copies. It also reduces response to TNF inhibitors.
Mucosal triggers — periodontal disease, lung exposures, gut dysbiosis
Porphyromonas gingivalis produces its own citrullinating enzyme and is enriched in early RA patients. Silica dust, textile dust, and other inhaled particulates also raise risk, supporting a mucosal-origin hypothesis for autoantibody generation.
Hormonal and reproductive factors
RA risk falls during pregnancy and rises in the postpartum period; nulliparity and early menopause increase risk, and oral contraceptives are weakly protective. The female-to-male ratio of 2-3:1 reflects this hormonal contribution.
Obesity and metabolic factors
BMI ≥30 raises RA risk by roughly 30% and worsens disease activity. Adipose tissue contributes inflammatory cytokines and reduces remission rates on standard DMARDs.
risk factors
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Living with it
01Stop smoking — the strongest modifiable risk factor; lowers risk especially in those with HLA-DRB1 shared epitope and improves DMARD response if disease develops
02Maintain healthy weight; BMI ≥30 raises RA risk by roughly 30% and reduces the likelihood of reaching remission on DMARDs
03Maintain good oral health and treat periodontitis aggressively — Porphyromonas gingivalis is implicated in autoantibody generation
04Limit occupational exposure to silica, textile dust, and solvents where feasible; use protective equipment where exposure is unavoidable
05Update vaccinations before any planned immunosuppression — pneumococcal (PPSV23 or PCV20), recombinant zoster (Shingrix), annual influenza, COVID-19, and hepatitis B as indicated
recommended foods
•Mediterranean diet rich in olive oil, vegetables, legumes, whole grains, and fish
•Oily fish (salmon, mackerel in moderation, sardines) 2-3 times weekly for omega-3 intake
•Walnuts, flaxseed, and chia seeds as plant sources of omega-3
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When to seek help
why see a rheumatology
A rheumatologist should be seen within six weeks of persistent inflammatory joint symptoms — early DMARD initiation within this window is the single strongest predictor of long-term remission and prevention of joint damage. Specialist input is also required for selecting and rotating biologics or JAK inhibitors, managing pregnancy in RA, evaluating extra-articular complications (interstitial lung disease, scleritis, vasculitis), and coordinating care with cardiology and pulmonology when complications develop.
01Joint deformity and erosive damage causing permanent loss of function — preventable with sustained low disease activity or remission
02Accelerated cardiovascular disease with roughly 50% increased mortality, driven by chronic inflammation and shared traditional risk factors
03Interstitial lung disease in approximately 10% of patients, more common in seropositive disease, smokers, and men; presents with breathlessness and dry cough
04Secondary Sjögren's syndrome with dry eyes and dry mouth in up to 30% of long-standing RA patients
05Osteoporosis and fragility fractures from chronic inflammation and glucocorticoid exposure; baseline DEXA and supplementation are standard
Seropositive RA (RF and/or anti-CCP positive)Roughly 70-80% of patients are RF positive and ~70% are anti-CCP positive. Seropositive disease tends to be more aggressive, erosive, and more often extra-articular.
Seronegative RARF and anti-CCP negative but clinical and imaging features meet criteria. Often milder course but can still erode joints; overlap with peripheral spondyloarthritis must be considered.
Elderly-onset RAFirst episode after age 65, often with large-joint involvement (shoulders), more abrupt onset, and overlap with polymyalgia rheumatica. Constitutional symptoms are prominent.
Palindromic rheumatismEpisodic monoarticular or oligoarticular attacks lasting hours to days with complete resolution between episodes. Roughly half progress to classic RA within five years, especially in anti-CCP positive patients.
Rheumatoid arthritis with extra-articular manifestationsIncludes Felty's syndrome (RA + splenomegaly + neutropenia), rheumatoid lung disease, vasculitis, and secondary Sjögren's. Predicts worse prognosis and higher mortality.
Living with Rheumatoid Arthritis
Timeline
Methotrexate begins to reduce symptoms over 6-8 weeks, with full response by 3-4 months; biologic DMARDs typically show benefit within 2-12 weeks depending on agent. A treat-to-target visit at three months guides escalation if the target is not met. Sustained remission, once achieved, is reviewed every six months; DMARD tapering may be considered after six to twelve months of sustained remission, though most patients require some maintenance therapy long-term to prevent relapse.
Lifestyle
01Engage in regular low-impact aerobic exercise (cycling, swimming, walking) for at least 150 minutes per week — improves function, fatigue, and cardiovascular risk without worsening disease
02Incorporate resistance training twice weekly under physical therapy guidance to protect muscle mass around vulnerable joints
03Adopt a Mediterranean-style eating pattern and reduce ultra-processed food intake; improves cardiovascular risk profile already elevated by RA
04Stop smoking and limit alcohol while on methotrexate or leflunomide — both increase hepatotoxicity risk
05Track disease activity with a simple home diary of stiffness duration, swollen joint count, and fatigue between visits
06Use occupational therapy aids — jar openers, kitchen knife handles, ergonomic keyboards — to reduce joint stress on the hands
07Prioritise sleep and pace activities to manage fatigue, which is often the most disabling symptom even when joint inflammation is controlled
Complementary approaches
Omega-3 fatty acids (2.7-3 g EPA+DHA daily)Meta-analyses including Goldberg 2007 and subsequent trials show modest reduction in morning stiffness and tender joint count after 3-4 months. Adjunctive to, not a replacement for, DMARDs.
Mediterranean dietary patternObservational and small interventional data (Sköldstam 2003) link Mediterranean-style eating to lower disease activity scores and improved physical function in RA.
Tai chi and yogaCochrane reviews show modest improvements in pain, stiffness, and physical function with regular practice. Useful as adjuncts to standard care and structured physical therapy.
Choosing a doctor
Look for board certification in rheumatology, experience with treat-to-target protocols using standardized disease activity scores (DAS28, CDAI, or SDAI), familiarity with biologic and JAK inhibitor selection including the post-ORAL Surveillance safety considerations, in-house musculoskeletal ultrasound capability, and clear care pathways with cardiology, pulmonology, and obstetrics. Continuity matters — RA is a multi-decade relationship, and the same clinician tracking trends in disease activity scores and imaging produces better outcomes than fragmented care.
Rheumatoid arthritis is not curable, but it is highly controllable with modern treatment. The goal is sustained remission or low disease activity using disease-modifying drugs such as methotrexate, biologics, or JAK inhibitors. Most patients diagnosed and treated early reach remission within 6-12 months and maintain it for years. Stopping medication entirely usually leads to relapse, so therapy is generally lifelong.
What are the first signs of rheumatoid arthritis?▾▴
The earliest signs are persistent morning stiffness lasting over 60 minutes, symmetric swelling and tenderness in the small joints of the hands and feet, and unexplained fatigue. Many patients also notice reduced grip strength and difficulty making a fist. Symptoms that last more than six weeks across multiple joints should prompt urgent referral to a rheumatologist.
How is rheumatoid arthritis diagnosed?▾▴
Diagnosis combines history, physical examination of tender and swollen joints, blood tests (rheumatoid factor, anti-CCP antibodies, ESR, CRP), and imaging (X-rays, ultrasound, or MRI). The 2010 ACR/EULAR classification criteria score joint count, serology, acute-phase reactants, and symptom duration. A rheumatologist confirms the diagnosis and rules out other causes of inflammatory arthritis.
What is the difference between rheumatoid arthritis and osteoarthritis?▾▴
Rheumatoid arthritis is autoimmune, symmetric, affects mostly small joints (MCPs, PIPs, wrists, MTPs), causes morning stiffness over an hour, and produces elevated inflammatory markers and often positive anti-CCP. Osteoarthritis is degenerative, often asymmetric, affects weight-bearing joints and the distal interphalangeal joints, causes brief morning stiffness under 30 minutes, and shows normal blood tests.
What is the best first-line treatment for rheumatoid arthritis?▾▴
Methotrexate is the anchor first-line treatment recommended by both the 2021 ACR and 2022 EULAR guidelines. It is started at 7.5-15 mg once weekly and titrated up to 25 mg weekly within two months, taken with folic acid to reduce side effects. About 40-50% of patients respond well to methotrexate alone within six months.
What does anti-CCP positive mean?▾▴
Anti-CCP positive means antibodies against cyclic citrullinated peptides were detected in the blood. This test is roughly 95% specific for rheumatoid arthritis and a positive result strongly supports the diagnosis. Anti-CCP positivity also predicts more aggressive, erosive disease and usually prompts earlier and more intensive DMARD treatment.
Can rheumatoid arthritis go into remission?▾▴
Yes. Sustained remission, defined as DAS28 below 2.6 or CDAI ≤ 2.8, is achieved by roughly 40-60% of patients in modern registries within the first 1-2 years of treat-to-target therapy. Remission is more likely with early diagnosis, methotrexate combined with biologics or JAK inhibitors as needed, and consistent monitoring every three months.
Are biologics safe long-term?▾▴
Biologics such as TNF inhibitors, tocilizumab, abatacept, and rituximab have decades of registry safety data and are well tolerated by most patients. The main long-term risks are serious infections, reactivation of latent tuberculosis or hepatitis B, and a small increase in certain skin cancers. Screening before starting and routine monitoring keep these risks low.
What is the JAK inhibitor boxed warning about?▾▴
After the ORAL Surveillance trial in 2022, the FDA added a boxed warning to tofacitinib, baricitinib, and upadacitinib for major cardiovascular events, malignancy, blood clots, and mortality in patients aged 50 and older with at least one cardiovascular risk factor. ACR 2021 now recommends a TNF inhibitor first in such patients, reserving JAK inhibitors for those who fail or cannot tolerate it.
Can women with rheumatoid arthritis have a healthy pregnancy?▾▴
Yes. Most women with rheumatoid arthritis have successful pregnancies, and RA often improves during pregnancy with flare in the postpartum period. Methotrexate and leflunomide must be stopped before conception, but hydroxychloroquine, sulfasalazine, and certolizumab pegol are considered safe during pregnancy. Preconception planning with a rheumatologist and obstetrician is essential.
Does smoking make rheumatoid arthritis worse?▾▴
Yes, strongly. Smoking is the strongest modifiable risk factor for developing RA, raises the chance of severe seropositive disease, increases joint damage, doubles the risk of interstitial lung disease, and reduces the response to TNF inhibitors. Stopping smoking improves DMARD response and lowers cardiovascular risk, which is already elevated in RA.
How long does it take for RA treatment to work?▾▴
Methotrexate begins to reduce stiffness and swelling within 4-6 weeks and reaches full effect by three months. Biologics typically work within 2-12 weeks depending on the agent. Glucocorticoids work within days and are used as a short bridge while DMARDs take effect. Disease activity is reassessed at three months and treatment escalated if the target is not met.
What joints does rheumatoid arthritis usually affect first?▾▴
The small joints of the hands and feet are usually affected first — particularly the metacarpophalangeal (MCP) joints, proximal interphalangeal (PIP) joints, wrists, and metatarsophalangeal (MTP) joints. The distal interphalangeal (DIP) joints of the fingers are characteristically spared, which helps distinguish RA from osteoarthritis. Disease is typically symmetric on both sides of the body.
Does rheumatoid arthritis shorten life expectancy?▾▴
Untreated and poorly controlled RA shortens life expectancy by roughly 5-10 years, mainly through accelerated cardiovascular disease and a higher rate of certain cancers and infections. With modern treat-to-target therapy and active management of cardiovascular risk factors, this gap has narrowed substantially and continues to shrink in registry data.
What happens if rheumatoid arthritis is left untreated?▾▴
Untreated RA progresses to permanent joint erosion within months, producing deformity (ulnar deviation, swan-neck and boutonnière deformities, hammer toes), loss of grip strength, and functional disability. Systemic complications including interstitial lung disease, accelerated atherosclerosis, vasculitis, and increased lymphoma risk also emerge. Early DMARD treatment within the first six months largely prevents this trajectory.
Can children get rheumatoid arthritis?▾▴
Children develop juvenile idiopathic arthritis (JIA), which is a related but distinct group of conditions starting before age 16. A small subset of JIA, called RF-positive polyarticular JIA, behaves similarly to adult RA. Pediatric rheumatologists manage these conditions and overall outcomes have improved markedly with biologic DMARDs.
What is the cost of rheumatoid arthritis treatment?▾▴
Methotrexate is inexpensive — usually under USD 20 per month as a generic. Brand-name biologics such as adalimumab and etanercept run roughly USD 50,000-80,000 per year in the United States; biosimilars typically reduce this by 30-50%. JAK inhibitor pricing varies. In India and other emerging markets, biosimilars are widely available at much lower prices, and insurance and patient assistance programs cover much of the cost elsewhere.
Should I exercise with rheumatoid arthritis?▾▴
Yes. Regular low-impact aerobic exercise such as cycling, swimming, and walking, combined with twice-weekly resistance training, improves pain, function, fatigue, and cardiovascular risk in RA. Exercise does not damage joints with active inflammation when sensibly graded. During an acute flare in a single joint, rest that joint while keeping the rest of the body active.
Do I need vaccinations before starting biologics?▾▴
Yes. Before starting biologics or JAK inhibitors, vaccinations should be updated where possible. Recommended vaccines include pneumococcal (PPSV23 or PCV20), recombinant zoster vaccine, annual influenza, COVID-19, and hepatitis B if not already immune. Live vaccines should generally be given before, not during, immunosuppression. Screening for latent tuberculosis and hepatitis B is also required before biologic therapy.
What is treat-to-target in rheumatoid arthritis?▾▴
Treat-to-target is a strategy where a specific disease activity goal — usually remission (DAS28 below 2.6) or low disease activity — is set, measured every three months with a standardized score, and treatment escalated whenever the target is not met. This approach, endorsed by ACR 2021 and EULAR 2022, consistently produces better outcomes than usual care.
When should I see a rheumatologist for joint pain?▾▴
See a rheumatologist within six weeks if you have persistent symmetric joint swelling, morning stiffness lasting over 30-60 minutes, or new positive RF or anti-CCP on blood tests. Early specialist evaluation matters because starting DMARDs within the first 3-6 months of symptom onset is the strongest predictor of long-term remission and prevention of permanent joint damage.
Persistent fatigue out of proportion to activity, often present months before joint pain becomes evident, and a leading patient-reported symptom in surveys.
05Low-grade fevers, weight loss, and malaise during active flares, reflecting the systemic inflammatory nature of the disease.
06Wrist pain and swelling with reduced grip strength — wrist involvement is present in over 75% of patients within the first two years.
07Foot pain on first weight-bearing in the morning from MTP synovitis; many patients describe walking on pebbles.
08Tendon involvement causing trigger finger, de Quervain's tenosynovitis, or extensor tendon rupture over the dorsum of the wrist.
09Late deformities including ulnar deviation at the MCPs, swan-neck and boutonnière deformities of the fingers, and hammer toes — reflecting cumulative cartilage and ligament damage rather than active inflammation.
10Rheumatoid nodules — firm, painless subcutaneous nodules over pressure points such as the olecranon, Achilles tendon, or extensor surfaces of the forearm — present in roughly 20-30% of seropositive patients.
11Dry eyes and dry mouth from secondary Sjögren's syndrome, present in up to 30% of long-standing RA patients.
12Cervical spine pain or new neurologic symptoms from atlantoaxial subluxation in advanced disease — uncommon today but warrants imaging if suspected.
early warning signs
•Persistent morning stiffness longer than 30 minutes for more than six weeks, especially across both hands
•Swelling around two or more small joints (MCPs, PIPs, MTPs) that does not resolve in days
•New onset of fatigue, low-grade fever, or unexplained weight loss alongside joint discomfort
•Positive rheumatoid factor or anti-CCP antibody on routine bloodwork ordered for vague joint symptoms
•Difficulty making a fist, opening jars, or wringing out a cloth that develops over weeks rather than years
● emergency signs
•Sudden severe pain, swelling, and fever in one joint of a patient already known to have RA — septic arthritis must be excluded urgently by aspiration
•New neurologic deficit, sensory loss in the limbs, or bladder/bowel changes in established RA — possible cervical myelopathy from atlantoaxial subluxation requiring imaging
•Sudden breathlessness, cough, or chest pain — possible RA-associated interstitial lung disease, pulmonary embolism, or pericarditis
•Painful red eye with vision change — possible scleritis, which can lead to ocular perforation if untreated
•Fever, mouth ulcers, or unusual infection in a patient on methotrexate, biologics, or JAK inhibitors — possible drug-induced cytopenia or serious infection
03
Erythrocyte sedimentation rate (ESR) and C-reactive protein (CRP)Acute-phase reactants reflecting inflammation. Used for diagnosis (one of the four ACR/EULAR criteria domains) and ongoing monitoring of disease activity and treatment response.
04
Plain radiographs of hands and feetEstablish baseline structural damage and detect periarticular osteopenia, joint space narrowing, and erosions. Repeated every 1-2 years to monitor radiographic progression.
05
Musculoskeletal ultrasoundSensitive detection of subclinical synovitis, tenosynovitis, and early erosions. Useful when examination is equivocal and to monitor response to therapy at the joint level.
06
MRI of hands or wristsMost sensitive imaging for bone marrow edema, synovitis, and pre-erosive change. Reserved for early or atypical cases where the diagnosis is uncertain.
07
Complete blood count and metabolic panelDetect anemia of chronic disease, thrombocytosis, neutropenia (Felty's), abnormal liver enzymes, and kidney function — baseline information that also guides DMARD selection.
08
Hepatitis B, hepatitis C, and tuberculosis screeningMandatory before starting biologics or JAK inhibitors that can reactivate latent infection. Screening usually includes HBsAg, anti-HBc, anti-HCV, and a TB interferon-gamma release assay (IGRA) or tuberculin skin test.
Outlook
With early diagnosis and modern treat-to-target therapy, the majority of patients now achieve low disease activity or remission, and structural damage is far less common than in pre-biologic decades. Sustained remission rates approach 40-60% in registry data within the first 1-2 years of treatment, and most patients maintain work and daily function. Despite this, RA still carries roughly 50% increased cardiovascular mortality through accelerated atherosclerosis and doubles the risk of lymphoma; aggressive disease control, smoking cessation, and cardiovascular risk management partially offset this excess. Key predictors of worse prognosis include seropositivity for both RF and anti-CCP, early erosions on imaging, high baseline disease activity, smoking, female sex, and lower socioeconomic status. The strongest predictor of a favorable long-term outcome is DMARD initiation within the first three to six months of symptom onset, underscoring the value of urgent specialist referral for new inflammatory joint pain.
Female sexnon-modifiable
Women are 2-3 times more likely to develop RA than men; lifetime risk is roughly 3.6% in women versus 1.7% in men.
Age 40-60 at onsetnon-modifiable
Incidence peaks in middle age, though RA can occur at any age. Elderly-onset disease has its own pattern with larger joint involvement.
Family history of RA or autoimmune diseasegenetic
First-degree relatives have a 3-5 fold increased risk. HLA-DRB1 shared epitope alleles carry the strongest single-locus effect.
Cigarette smokingmodifiable
Heavy smoking with HLA-DRB1 shared epitope raises anti-CCP positive RA risk up to 20-fold and lowers remission rates and TNF inhibitor response.
Periodontal disease and Porphyromonas gingivalis carriagemodifiable
Periodontitis is more common in pre-clinical and early RA; the bacterium uniquely produces a citrullinating enzyme implicated in autoantibody formation.
Obesity (BMI ≥30)modifiable
Raises RA incidence by roughly 30% and reduces the chance of reaching remission on DMARDs by approximately 50% in some cohorts.
Occupational exposure to silica, textile dust, or solventsenvironmental
Inhaled silica raises RA risk 2-3 fold and is recognized as an occupational cause in many jurisdictions; textile dust exposure shows similar associations.
Lower socioeconomic status and lower educational attainmentenvironmental
Linked to higher RA incidence and worse disease activity, partly mediated by smoking, occupational exposures, and delayed access to specialist care.
Postpartum periodnon-modifiable
RA onset and flare are more common in the first 3-12 months after childbirth; pregnancy itself often produces temporary improvement.
•
Coffee in moderation — no consistent harm signal in modern cohorts
•Fermented dairy products such as yogurt and kefir; some evidence for gut microbiome benefit
•Calcium and vitamin D rich foods to offset glucocorticoid-related bone loss
foods to avoid
•Excessive red and processed meat — linked to higher disease activity and cardiovascular risk
•Sugar-sweetened beverages and ultra-processed foods which worsen metabolic and inflammatory profile
•Alcohol while taking methotrexate or leflunomide because of additive hepatotoxicity
•High-sodium diets that worsen blood pressure on glucocorticoids and NSAIDs
•Unproven elimination diets that risk nutritional deficiency without measured benefit
•Raw or undercooked animal products in patients on biologics or JAK inhibitors to reduce infection risk
06
Felty's syndrome — RA with splenomegaly and neutropenia — uncommon today but raises infection risk significantly
07Lymphoma at roughly twice the general population risk, especially with high cumulative disease activity
08Cervical spine instability with atlantoaxial subluxation in long-standing erosive disease, occasionally producing myelopathy
09Serious infections related to immunosuppressive therapy — opportunistic infections, herpes zoster reactivation on JAK inhibitors, and tuberculosis or hepatitis B reactivation on biologics
01Take DMARDs and biologics on schedule — methotrexate on the same weekday each week, with a separate folic acid day
02Track stiffness duration, swollen joints, fatigue, and any new symptoms weekly so trends can guide treatment decisions
03Maintain consistent low-impact activity even on stiff days; movement reduces stiffness more reliably than rest
04Apply joint protection principles at work and home — larger handles, two-handed lifting, alternating tasks
05Carry an up-to-date medication list and biologic injection schedule, including the date of the next infusion or self-injection, to share with any emergency or surgical team
Exercise
Regular aerobic and resistance exercise is safe and beneficial in RA, including during periods of low disease activity. Aim for 150 minutes per week of moderate aerobic activity combined with twice-weekly resistance work. Hydrotherapy and warm-water exercise are well tolerated when joints are tender. During an acute flare in a single joint, rest and ice that joint while keeping the rest of the body active; complete bed rest worsens fatigue and deconditioning.