EDITORIAL

Rheuminations
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Prashant Kaushik ,  Aarya A. Kaushik

I'll be honest…it has been 35+ years since I started 
Medical School [MBBS]. And in the realm of 
Medicine at large, and Immunology/Rheumatology 
in specific, we are still struggling to find a 'cure' for 
chronic systemic inflammatory immune-mediated 
diseases also known as 'autoimmune rheumatic 
diseases (ARD)'. Rheumatology is still in its cradle 
having gotten the recognition as a subspecialty of 
Medicine only in 1972. I have seen the field evolve in 
terms of understanding the orchestrated 'play' of the 
immune cells along with cytokines etc. over the past 
3 decades, all of which has led to the concept and 
birth of 'biologic' disease modifying anti-rheumatic 
drugs [b-DMARDs]. The first b-DMARD to get 
approved by the Food and Drugs Administration 
[FDA] was etanercept, a TNF-alpha receptor fusion 
protein in 1998. Infliximab, a chimeric monoclonal 
antibody against TNF soon followed in 1999. Ever 
since then, there has been a flurry of b-DMARDs 
including 3 more in the same family of TNF-
antagonists, 2 in the Interleukin [IL]-6 antagonist 
class, 1 blocker of the second co-stimulatory T-cell 
signaling: CTLA-4Ig, 3 IL-1 antagonists, B-cell 
depleting chimeric monoclonal antibody directed 
against CD-20 etc. Also, 3 oral Janus-kinase inhibitors 
have joined the 'gang' and are called targeted 
synthetic DMARDs. 
I still remember the pre-b-DMARD era when rip 
roaring rheumatoid arthritis was still around, and 
with my Ustaad Saheb (Mentor), all what we had to 
offer pharmaceutically were the conventional 
synthetic [cs] DMARDs including methotrexate, 

hydroxychloroquine, sulfasalazine, leflunomide and 
[the younger generation can hold their breath] 
cyclosporine, d-penicillamine, chlorambucil…GOLD 
i n j e c t i o n s  a n d  e v e n  c y c l o p h o s p h a m i d e !  

st
Corticosteroids have been around since 1950! The 1  
and “so far” […well, I/You might be next one!] the 
only Nobel Prize winning revelation in the realm of 
Rheumatology. 
The availability of the b-DMARDs has changed the 
entire paradigm of pharmaceutical treatment in 
Rheumatology. They are all quite effective yet 
extremely expensive making them literally 
unaffordable in the parts of the world, where health-
insurance coverage is suboptimal/non-existent, 
more so, given the indefinite duration of therapy. 
Although the b-DMARDs tend to target a specific 
pathway in the immune system, they are still fraught 
with some rather challenging adverse drug effects 
(ADE) including infections:  bacterial, mycobacterial 
[especially reactivation of tuberculosis, more so, in 
the parts of the world where this disease is endemic] 
fungal and from other pathogens; malignancies, 
increased incidence of cardiovascular and 
cerebrovascular events, thromboembolic events etc. 
All in all, b-DMARDs are a double-edged sword! They 
all come with 'a price to pay'!
Now, let's reflect upon the burden of ARD in the 
community. Rheumatoid arthritis, a potentially 
crippling and life-threatening disease affects at least 
1% of the population, with more than 13 million 
patients in America itself! Axial and peripheral 
spondyloarthritis is now being recognized more and 
more. Various other autoimmune diseases including 
systemic lupus erythematosus, Sjogren's syndrome, 
scleroderma, autoimmune myopathy including 
dermatomyositis and polymyositis, vasculitides, and 
some more novel entities like IgG-4 related disease, 
checkpoint-inhibitor chemotherapy associated 
rheumatic diseases: the list continues to grow! 
What can be done to prevent, slow, stop and reverse 
ARD? In fact, the answer is the other side of the 
question itself! Human body has a tremendous 
capacity of healing itself! Only, if we are willing to 
make healthy choices. Truth is Self-effulgent! It does 

Correspondence:
Dr. Prashant Kaushik, MBBS
Chief of Rheumatology, NHS, Tahlequah, OK
Associate Professor of Medicine, OSU CHS CN
Associate Program Director, IM residency, NHS
E-mail: prashantkaushik2508@gmail.com

Received: November 29,2022; Accepted: December 14, 2022

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1
Prashant Kaushik MBBS, MNAMS, FACP, FACR, Rh MSUS

2
Aarya A. Kaushik

A.B. Candidate '24, Harvard University
English and Music 
Secondary in Global Health and Health Policy 
Staff Writer, The Harvard Crimson 
Poetry Editor, The Harvard Advocate 
Research Associate, Joslin Diabetes Center

DOI: https://doi.org/10.57234/1621



not require a lab-proof! However, as 'scientists', we 
are always inclined to see/measure the outcomes. 
Well, it is out there now! SYSTEMIC INFLAMMATORY 
DISEASES CAN BE PREVENTED AND REVERSED!!! 
Here are the revelations about some of these 
ailments including coronary heart disease, diabetes 
mellitus and even prostate cancer from just a few 
extremely humbling articles published quite 
recently.
The Lifestyle Heart Trial showed that it is possible to 
significantly reduce coronary stenoses and risk of 
cardiac events using aggressive lifestyle changes, and 
without lipid-lowering medications. A strong dose-
response relationship between self-reported 
adherence and angiographic changes was found, 
with excellent adherence during the study. Overall, 
self-reported adherence was highly correlated with 

1
percentage of stenosis. It has also been shown that  
an intense lifestyle treatment can reduce the 

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expenses on cardiac health/procedures drastically.  
Interestingly, adherence to a whole food plant-based 
nutritional program was found to be more important 
than the type of diet consumed.  More adherent 
subjects showed greater improvements in weight 
and cardiac parameters.  Thus, the intensity of the 
intervention may be more important than the 

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specific diet for weight loss.  
By limiting the daily caloric consumption to 600 
C a l o r i e s ,  d e c r e a s e d  p a n c r e a t i c  a n d  l i v e r  
triacylglycerol stores, improved maximal insulin 

4  
sensitivity.  It's very humbling! , a 12-The DIETFITS
month randomized clinical trial demonstrated that 
epigenetics must be part of the measures assessed in 
lifestyle diet intervention studies.  Diet determines 

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the expression of many genes!  
The Direct study was the first large rigorous trial to 
show such success in remission of diabetes in a 
clinical practice setting. Diabetes-remission was 
strongly associated with weight loss in a dose 

 6,7
response relationship.
A fasting-mimicking diet (FMD) demonstrated that 
the power of dietary interventions may include 
reprogramming of tissues to restore lost metabolic 
function, such as beta cells in the pancreas.  Once 
confirmed in humans, this could elevate lifestyle 
medicine intervention as a 'primary' modality for 
type 2 diabetes mellitus treatment.  Also, should this 
treatment lead to beta-cell neogenesis in humans, it 

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could make type 1 diabetes mellitus reversible.
From diabetes 'care' to diabetes 'cure': In a seminal 
article published about 5 years ago, creative ways to 
implement lifestyle interventions were reiterated. 
Those services would include coaching, information, 

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and communications technology.
Intensive nutrition and lifestyle changes can even 

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modulate gene expression in the prostate cancer.
So, in a nutshell, ALL chronic lifestyle mediated 
diseases have systemic inflammation, alteration in 
the gut microbiome, oxidative stress, allostatic load, 
and many other features in common! Well, then the 
answer becomes simple! It is possible to prevent, 
slow, stop the progression and even reverse all these 
diseases with 'the exact same' 4-pronged approach: 
eat well, move more, think right, and love ALL! The 
s a g e  g e n e r a t i o n a l  w i s d o m  o f  D a d i / N a n i  
(grandmothers) has no ADE!
It's work, yes, but 'its works'!

REFERENCES
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PMC5357144.

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PMC5786854.

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