Friday, May 8, 2026

“The Story of My Life” – An Autobiography of NSAID

Hello…

I am an NSAID — a Non-Steroidal Anti-Inflammatory Drug.

You may know me through many names:

πŸ’Š Ibuprofen
πŸ’Š Diclofenac
πŸ’Š Naproxen
πŸ’Š Aspirin
πŸ’Š Aceclofenac

Whenever pain, swelling, fever, or inflammation troubles the human body, I often arrive quietly… but powerfully.

But my story is not just about relief.
It is a fascinating biochemical journey inside the human body.

Come with me, and I will show you how I fight pain through the inhibition of COX enzymes and prostaglandin synthesis.

🧬 Chapter 1 – The Alarm Begins

My story starts when the body faces:

  • Injury
  • Infection
  • Tissue damage
  • Arthritis
  • Muscle strain

The moment cells are injured, the cell membrane becomes disturbed.

Suddenly, an enzyme awakens:

πŸ”₯ Phospholipase A₂

Its mission?
πŸ‘‰ To release a hidden fatty acid from membrane phospholipids:

Arachidonic Acid

This molecule is the starting point of inflammation.

⚙️ Chapter 2 – The Arachidonic Acid Pathway

Once released, arachidonic acid enters an important biochemical pathway.

One road leads to:

πŸ§ͺ Cyclooxygenase (COX) Enzymes

These enzymes are the architects of inflammatory mediators.

There are two major forms:

πŸ”΅ COX-1 — The Protector

COX-1 is always present in the body.

It performs important protective functions:

✔ Protects stomach lining
✔ Maintains kidney blood flow
✔ Supports platelet aggregation
✔ Produces protective prostaglandins

COX-1 is not harmful.
In fact, it is essential for normal physiology.

πŸ”΄ COX-2 — The Inflammatory Trigger

COX-2 appears mainly during:

  • Injury
  • Infection
  • Cytokine stimulation
  • Inflammation

It produces prostaglandins responsible for:
πŸ”₯ Pain
πŸ”₯ Swelling
πŸ”₯ Fever
πŸ”₯ Redness

And this is where I step into action.

πŸ§ͺ Chapter 3 – Birth of Prostaglandins

The COX enzymes convert arachidonic acid into unstable intermediates:

Arachidonic Acid

into unstable intermediates:

  • PGG₂
  • PGH₂

These intermediates are transformed into:

MediatorFunction
PGE₂Pain and fever
PGI₂Vasodilation and inflammation
TXA₂Platelet aggregation
PGF₂Ξ±Smooth muscle contraction

Among them, PGE₂ becomes one of the major causes of inflammatory pain and fever.

πŸ’Š Chapter 4 – My Mission Begins

I enter the bloodstream after administration.

My target?

🚫 Cyclooxygenase (COX)

I bind to the enzyme and inhibit its activity.

The mechanism is simple but powerful:

NSAIDs+COX enzyme→↓Prostaglandin synthesis

As prostaglandin production decreases:
✔ Pain reduces
✔ Fever falls
✔ Inflammation subsides

The biochemical storm begins to calm.

πŸ’₯ Chapter 5 – My Analgesic Effect (Pain Relief)

During inflammation, prostaglandins sensitize pain receptors.

Especially:

πŸ”₯ PGE₂

It tells nerves:
⚠️ “Feel more pain!”

I stop this message by reducing prostaglandin synthesis.

Result:
✔ Less sensitivity of nociceptors
✔ Reduced headache
✔ Relief from joint and muscle pain

That is my:

πŸ’₯ Analgesic Action

🌑️ Chapter 6 – My Antipyretic Effect (Fever Reduction)

During infections, pyrogens stimulate prostaglandin synthesis in the hypothalamus.

PGE₂ increases the body’s temperature set point.

I inhibit hypothalamic prostaglandin production

Result:
✔ Body temperature normalizes
✔ Fever decreases

That becomes my:

🌑️ Antipyretic Action

πŸ”΄ Chapter 7 – My Anti-inflammatory Effect

Inflammatory prostaglandins cause:

  • Vasodilation
  • Swelling
  • Redness
  • Increased vascular permeability

By blocking COX enzymes:
πŸ‘‰ I reduce inflammatory mediator production.

Result:
✔ Reduced edema
✔ Improved mobility
✔ Relief in arthritis and injuries

That is my:

πŸ”₯ Anti-inflammatory Action

⚠️ Chapter 8 – My Limitations

But every powerful medicine has risks.

When I inhibit COX-1 excessively:
⚠️ Gastric irritation occurs
⚠️ Ulcers may develop
⚠️ Kidney blood flow decreases
⚠️ Bleeding tendency may increase

Especially during:

  • High doses
  • Long-term use
  • Self-medication

That’s why I always say:
πŸ‘‰ “Respect dosage and medical guidance.”

🧬 Chapter 9 – My Evolution

Scientists wanted safer versions of me.

So they developed:

🟒 Selective COX-2 Inhibitors

Examples:

  • Celecoxib
  • Etoricoxib

These selectively block inflammatory COX-2 while sparing protective COX-1.

Advantages:
✔ Less gastric toxicity

But even these newer forms have challenges:
⚠️ Increased cardiovascular risks

Science continues to refine us.

🌍 Chapter 10 – My Life Today

Today, I am one of the most widely used drug classes in the world.

I help millions suffering from:

  • Arthritis
  • Fever
  • Dental pain
  • Sports injuries
  • Postoperative inflammation

From clinics to households…
my journey continues every day.

🧠 Chapter 11 -  Summary Flowchart

Result:

✔ Analgesic
✔ Antipyretic
✔ Anti-inflammatory actions

❤️ My Message

I am not merely a painkiller.

I am:
πŸ§ͺ A biochemical inhibitor
🧬 A controller of inflammatory mediators
πŸ’Š A regulator of prostaglandin synthesis

But with great power comes responsibility.

πŸ‘‰ Use me correctly
πŸ‘‰ Avoid misuse
πŸ‘‰ Respect science

Epilogue

From entering the bloodstream…
To blocking the COX pathway…
To silencing prostaglandins…

This is my story.

I am an NSAID — the quiet warrior against pain, fever, and inflammation.

at
Labels: , , , , ,

No comments:

Post a Comment

Subscribe to: Post Comments (Atom)

“The Story of My Life” – An Autobiography of NSAID

Hello… I am an NSAID — a Non-Steroidal Anti-Inflammatory Drug . You may know me through many names: πŸ’Š Ibuprofen πŸ’Š Diclofenac πŸ’Š Naproxen ...