photo dynamic therapy
DESCRIPTION
photodynamic therapy-the new way of treating cancer,its drugs,side effects,treatments,what is it? etc. etc :)TRANSCRIPT
PHOTO DYNAMIC THERAPY
-LALITHA KAVYA
INTRODUCTION It form of phototherapy using nontoxic light-sensitive
compounds that are exposed selectively to light, whereupon they become toxic to targeted malignant and other diseased cells.
PDT has proven ability to kill microbial cells including bacteria, fungi and viruses.
In PDT, the usage of the right wavelength of the light,the correct light-sensitive compounds which are at the same time highly effective to treat the targetted tissue is an important step that needs to be followed.
INTRODUCTION-WHY PDT?• It is the best alternative for extensive surgery.• It does not take long time.• It is minimally invasive therefore it saves recovery
time .(minimal recovery period).• It is minimally toxic.• Less scarring (when compared to the extensive
surgery)• Patient suffering due to pain post PDT is very
minimal.• Preparation time is also minimal.
KEY COMPONENTS• PDT has three essential components:-1. LIGHT SOURCE2. PHOTO SENSITIZER3. MOLECULAR OXYGEN• The obvious requirement for the action of PDT is a
TARGET TISSUE.
KEY COMPONENTS• PHOTO SENSITISER is a substance which absorbs the
wave length of the light focussed on it and inhibits photo reaction to other normal cells surrounding the tissue.
• Use of visible and near infra red light with a photo sensitiser to treat the diseased tissue.
• The wavelength of the light source needs to be appropriate for exciting the photosensitizer to produce REACTIVE OXYGEN SPECIES. combination of these three components leads to the chemical destruction of any tissues that have been exposed to this light.
PRINCIPLE A photo sensitiser is administered to theTargetted tissue (for example a tumor).Light isthen allowed to concentrate on this targettedtissue which is absorbed by the photo sensitiserand this causes the generation of reactiveoxygen species. • Example of photo sensitisers:-• PORFIMER SODIUM,AMINOLEVULINIC ACID
PDT-LASER
MECHANISM OF ACTION • The photosensitizer is excited from a ground singlet state
to an excited singlet state. It then undergoes intersystem crossing to a longer-lived excited triplet state.
• One of the few chemical species present with a ground triplet state is “MOLECULAR OXYGEN”. When the photosensitizer and an oxygen molecule are in proximity, an energy transfer can take place that allows the photosensitizer to relax to its ground singlet state, and create an excited singlet state oxygen molecule.
• Singlet oxygen is a very aggressive chemical species and will very rapidly react with any nearby biomolecules.
MECHANISM• Ultimately, these destructive reactions will kill
cells through apoptosis or necrosis.
• PDT can be considered a form of targeted ’singlet oxygen chemotherapy’where the targeting is achieved with the combination of the photosensitizer and intense light.
MECHANISM • Photosensitizer(p.s) Oxygen
Ground triplet state
Ground singlet state EXCITED SINGLET STATE
Excited singlet state
Excited triplet state
GROUND SINGLET STATE
INCIDENT LIGHT
Oxygen (excited singlet state)
P.S ( ground singlet
state)
TREATMENT-PORFIMER SODIUM• First, the porfimer sodium(photo sensitiser) is
administered intravenously into the cancer patient.• It travels through the bloodstream and is absorbed
by every cell in the body (both the normal and the cancerous cells).
• The normal cells get rid of porfimer sodium in a couple of days.But a lot of the drug stays in the cancer and normal skin cells.
• Porfimer sodium is activated or turned on by light (visible/infra red) after 2-3 days of administering it into the body.
• This gives normal cells to get rid of the drug.
TREATMENT-PORFIMER SODIUM• The doctor directs a laser light at the area of cancer
cells through a thin fiber optic glass strand.• LASER used is a low power light so it does not burn.It
gives minimal or no pain.• Depending on the size of the tumor,the light is given
from 5-40 minutes.• Any dead tissue left in the treated are is removed
after 4-5 days.• The treatment can be repeated.
TREATMENT-AMINOLEVULINIC ACID• Aminolevulinic acid is a topical drug applied directly
on skin to treat actinic keratosis (a pre malignant condition).
• It is a solution that is applied directly on face or scalp (unlike porfimer sodium,this does not reach other body parts).
• After 14-15 hours of application of the drug,doctor passes BLUE LIGHT onto the area for 15 minutes.
• The area may become red,scaly and crusty for almost 4 weeks before healing.
• If the lesion does not go away completely,it can be treated again after 8 weeks.
ACTINIC KERATOSIS
PDT-ADVANTAGES AND LIMITATIONS• PDT is considered to be both minimally invasive and
minimally toxic, these advantages alone make PDT an attractive alternative.
• Compared to radiotherapy, chemotherapy and surgical operation for the treatment of cancers, PDT is in almost all cases a much cheaper alternative.
• Furthermore, post-operative recovery after PDT is typically hours or days rather than weeks.
PDT-ADVANTAGES AND LIMITATIONS• It cannot be used to treat all types of cancers.• The photosensitisers in some cases,might be harmful
as the normal cells feed up on it and the patient’s eyes and skin might become very photo
sensitive for about 30 days.• The skin might burn or blister or swell if exposed to
direct sunlight.• The availability of PDT is scanty as research is still
going on about its applications and suitability in various geographical areas.
PDT-ITS RESULTS
PDT-ITS RESULTS
CONCLUSION• Photodynamic therapy is one of the best
techniques to cure many ailments which normal clinical techniques are inefficient in solving .
• In a few years its popularity and also availability to the common man is foreseen.
• It comes across as a very safe and potential way to solve cases of cancer, skin ailments etc.
• The awareness of photodynamic therapy is increasing rapidly and soon it will attain a position where it will be considered a “BOON” to the medical and scientific fields…
THANK YOU FOR YOUR TIME AND PATIENCE…