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Stephen G Bown National Medical Laser
Centre, Department of Surgery, University College London Medical
School, London W1P 7LD
From a medical point of view, lasers are a convenient but
sophisticated source of light in the visible, ultraviolet, and infrared parts of the spectrum. They are easy to control, and the light beam (of
a single colour) can be focused to a small spot and in many cases can
be transmitted via thin flexible fibres, making internal delivery of
light feasible. The range of clinical applications is enormous, from
the simple carbon dioxide laser, used as a non-contact scalpel or for
superficial tissue ablation, to the precision of the excimer laser,
used for reshaping corneas, and the flash lamp pumped dye laser, used
to close the small blood vessels of disfiguring port wine birthmarks.
This review looks at how the precision of light delivery and the
predictability of biological response possible with laser therapy is
starting to be exploited for the in situ destruction of diseased tissue
and how these techniques might be developed in the future.
The first requirement for successful clinical use of lasers is to
understand how light at the wavelength used can interact with living
tissue. Most of the simple applications are thermal, but the effect
produced depends on how much heat is delivered, how fast it is
delivered, and the volume of tissue in which it is absorbed.
Increasingly, however, the new technique of photodynamic therapy
(non-thermal effects from combining laser light and a photosensitising
drug) is attracting interest. This review considers particularly the
effects of low power thermal treatment and photodynamic therapy (see
table).
The carbon dioxide laser (wavelength 10 600 nm in the far
infrared) is well established as a non-contact scalpel in relatively inaccessible areas like the brain and upper airways and for ablating small lesions as on the skin. However, the beam cannot be transmitted via flexible fibres and can only produce haemostasis in vessels well
below 1 mm in diameter.
Light in the near infrared part of the spectrum The same principle (although with much less immediate vaporisation) is
applied to cystoscopic laser treatment of benign prostatic hypertrophy.
Special side firing laser fibres are used to direct the beam at the
urethral surface of the prostate under direct vision. This is fairly
widely used as an alternative to conventional transurethral resection,
particularly in North America. However, more sophisticated ways of
using these lasers are now emerging.
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Thermal laser therapy
Possible futures
Image guided laser treatments in minimally invasive destruction
of a wide range of tumours
Greater use of interstitial laser photocoagulation for lesions in solid
organs, with potential targets including benign prostatic hypertrophy
and small localised cancers or benign lesions of the liver, breast,
uterus, and other organs
Increased use of photodynamic therapy with potential targets including
dysplasia and localised tumours of the skin, mouth, oesophagus, major
bronchi, bladder, and vulva.
Other potential applications of photodynamic therapy include preventing
restenosis after balloon angioplasty or stent, to ablate the uterine
endometrium, as an adjunct to cancer surgery, and treating macular
degeneration and localised infections with resistant organisms
The next generation of reliable and cheap lasers will make most of
these techniques accessible to all large hospitals
as from a NdYAG
laser at 1064 nm or a semiconductor diode laser at 805 nm
penetrates tissue much better, producing effects through up to 10 mm of tissue. Immediately under a high power NdYAG laser beam, tissue is vaporised. Below the surface, tissue is coagulated, with effective haemostasis, and may later slough or heal with fibrosis. This beam can be
transmitted via thin fibres, so the technique is of particular value
for endoscopic palliative debulking of advanced cancers of the upper
and lower gastrointestinal tract and major airways. Used in conjunction with brachytherapy (single dose intraluminal radiotherapy), this can
provide excellent palliation for extended periods and is complementary to insertion of a stent.1 This application is relatively
crude, but well established and effective.
Interstitial laser photocoagulation
In this technique laser light is delivered to lesions in the
centre of solid organs via fibres positioned through needles inserted percutaneously under image guidance. At low power (typically about 3 W, so there is no tissue vaporisation, compared with the 60-80 W used endoscopically), the diseased tissue is gently coagulated over a few minutes in such a way that the dead tissue can be resorbed by normal healing mechanisms without the need for further intervention. There is no effect on the overlying normal tissue, no cumulative toxicity (so treatment can be repeated if necessary), and no surgical wound to heal so recovery is rapid. However, the keys to success are
positioning the fibres in the right place, matching the extent of laser
induced necrosis to the limits of the lesion being treated, and
ensuring that all treated areas (normal or abnormal) will heal safely.
The whole process is critically dependent on imaging.
The best established application is for
treating small, isolated metastases in the liver (mainly from
previously resected colorectal primary cancers) in patients who are
unsuitable for surgery.2 Under local anaesthesia and
sedation, the needles are inserted percutaneously under computed
tomographic guidance, the result being assessed on contrast enhanced
computed tomograms taken 24 hours later. The technique is more
controllable than percutaneous alcohol injection and simpler than
cryotherapy.
Breast cancer
The potential application attracting
most interest is using interstitial laser photocoagulation in the
initial treatment of small breast cancers as an alternative to
lumpectomy
this would leave no scar or cosmetic deformity and could be
a simple outpatient procedure performed under local anaesthetic.
Contrast enhanced magnetic resonance imaging is extremely good at
defining the limits of breast cancers and the limits of laser
induced necrosis in cancers treated with interstitial laser
photocoagulation a few days before definitive surgery.3
Further, if the procedure is undertaken with the patient in a magnetic
resonance imager, changes can be seen on the images as the laser is
firing, so the positions of the fibres can be adjusted if treatment is
incomplete or in the wrong place. However, there is a long way to go
before it will be clear whether interstitial laser photocoagulation can have a role in the routine management of breast cancer, as it is so
crucial to be sure that all the cancer has been destroyed before the
laser necrosed tissue can be safely left in situ.
Benign disease
The technique may have a role much sooner in
managing benign fibroadenomas of the breast. Many of these need no
treatment, but, for those that do, interstitial laser photocoagulation
is a simple alternative to excision that should leave no scar, which is
particularly attractive for patients inclined to formation of keloids.
Early results from clinical trials are promising. Similarly,
interstitial laser photocoagulation is being explored for treating
small, symptomatic uterine fibroids and as an alternative laser
technique for treating benign prostatic hypertrophy.4
In principle, interstitial laser photocoagulation is applicable to well defined lesions in any solid organ in which the effect can be well enough localised not to cause any unacceptable damage to the surrounding normal tissue.
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Photodynamic therapy |
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The form of light activated treatment that probably has the greatest overall potential is photodynamic therapy, although no applications are yet firmly established. This technique involves treatment with low power red light (usually from a laser) after administration of a photosensitising drug. There is no increase in tissue temperature. The real attraction is the nature of the tissue damage. Unlike thermal damage, connective tissues like collagen and elastin are largely unaffected, so there is much less risk to the mechanical integrity of hollow organs and healing takes place with more regeneration and less scarring. However, photodynamic therapy is more complicated as it involves delivery of both drug and light, and, for best results, close collaboration between scientists and clinicians is essential. 5 6
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Photodynamic therapy first attracted widespread attention because many photosensitisers are taken up slightly more by cancers than by the adjacent normal tissue. Unfortunately, the dream that this might be exploited to give selective necrosis of cancers without damaging adjacent tissues has not been realised, and, in general, the area necrosed is the area exposed to the light. Nevertheless, damage by photodynamic therapy in many normal tissues heals so well that the final result may effectively be selective necrosis of small tumours.
Neoplasia of hollow organs
Photodynamic therapy is probably most useful for early invasive
cancers in patients who are unsuitable for surgery. Most work has been
done on localised cancers of the oral cavity with photosensitisers like
porfimer sodium (Photofrin) and meso-tetra hydroxyphenyl chlorin (mTHPC, Foscan). These agents show no selectivity of necrotic effect between mucosa and underlying tissues, and the depth of necrosis
can be 5 mm or more, but treated areas heal remarkably well (see fig
1).7 Good results have been reported for endoscopic photodynamic therapy for small cancers of the major airways,
oesophagus, stomach, and colon, but it cannot treat tumour that has
spread beyond the wall of the organ of origin.8
Experimental work suggests that normal bone is remarkably resistant to
photodynamic therapy, so it may be a useful treatment for oral cancers
that have invaded the mandible or maxilla, avoiding the need for
mutilating surgery or radical radiotherapy.
Neoplasia of solid organs
Recently, research has focused on the potential of interstitial
photodynamic therapy with meso-tetra hydroxyphenyl
chlorin for treating cancers in solid organs, particularly the prostate and pancreas. As more early prostate cancers are being found in younger
asymptomatic men with an elevated blood level of prostate specific
antigen, so the need increases for a potentially curative treatment
that carries less risk of incontinence and impotence than radical
prostatectomy or radical radiotherapy. Clinical trials of laser therapy
have just started and are limited to patients with locally recurrent
cancers after radiotherapy, but in some the levels of prostate specific
antigen have been reduced to levels seen after radical prostatectomy
and the incidence of complications has been low. If photodynamic
therapy proves effective as primary treatment for localised disease
with a low incidence of complications then this could be an important
advance.
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Vascular disease
One of the main problems after balloon angioplasty or insertion of
a stent for obstructive vascular disease is restenosis, which is
related at least in part to proliferation of smooth muscle cells from
the media. Experiments have shown that photodynamic therapy with
5-amino laevulinic acid effectively suppresses this cell proliferation
without increasing the risk of thrombosis or weakening the mechanical
strength of the arterial wall.12 Clinical trials have just
started. Conventional balloon angioplasties of stenosed superficial
femoral arteries have been undertaken in photosensitised patients, and
the guide wire then replaced by a thin laser fibre to deliver light to
the treated area. The technique seems to be feasible and safe, but it
is too early to judge efficacy. Interest among cardiologists currently
centres on suppressing smooth muscle proliferation with brachytherapy
(local radiotherapy), but if photodynamic therapy could produce the
same effect it would be preferable as it would avoid the use of
ionising radiation. The potential of this application is enormous as it
could mean using photodynamic therapy as adjuvant treatment for most
endoluminal procedures on coronary and peripheral arteries.
Localised infections
Microorganisms are another potential target. Indeed, the first
description of photodynamic therapy dates back to 1900 in a story
reminiscent of the discovery of penicillin.14 Oscar Raab in Munich was assessing the toxicity of the dye acridine on
Paramecium. On a sunny day it was toxic, but not during
a great thunderstorm. He quickly realised the importance of light.
such as in
treating genital warts
as tissue necrosed by photodynamic therapy in
these areas heals so well with little scarring and treatment can be
repeated if necessary.
Menorrhagia
Photodynamic therapy could also be used to destroy essentially
normal tissue, and the procedure attracting most interest at present is
endometrial ablation to control menorrhagia. The idea is to inject the
photosensitiser directly into the uterine cavity and then activate it
by red light delivered by soft, flexible, optical devices that can be
easily and safely inserted through the cervix, preferably without
dilatation, to illuminate the entire endometrium.15 Many
techniques have been tried to control menorrhagia without the need for
hysterectomy, with varying degrees of success, and photodynamic therapy
is only just starting clinical trials. However, it does have the
advantages of not requiring advanced surgical skills and being unlikely
to damage any adjacent organs, as the low power red light used would
not penetrate through the myometrium. To take this procedure to its
logical conclusion, if photodynamic therapy could produce complete
endometrial ablation patients would probably become sterile. If this
proved safe and reliable, it would be a simple and cheap method for
female sterilisation that could rapidly be made available almost
anywhere.
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Conclusions |
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Clinical lasers used to be large, expensive, unreliable, and difficult to operate. Many are now the size of a briefcase, can be plugged into a standard power socket, and are rugged enough to be easily moved between locations for many uses. As demand increases, so the price is coming down.
For low power applications in which transmission of the light by fibre is not essential (as for photodynamic therapy of the skin and some internal sites where it may be possible to use a broader light delivery system such as in the mouth and the uterine endometrium), cheaper non-laser sources can be used such as light emitting diodes (LEDs) and suitably filtered beams from a xenon lamp. Thus, many of the future treatments suggested here could become accessible to most hospitals. The ones that would have to stay in specialist centres are those requiring sophisticated image guidance such as the treatment of breast, prostate, and pancreatic cancers.
Most of the new applications of lasers described here are already in early clinical trials. Others are more speculative, but for all, the basic validity of the required biological effects has been established. Work is still needed to identify which applications will find a place in routine medical practice and how these techniques will compare with other therapeutic options. Nevertheless, the evidence is mounting that laser treatments can offer considerable advantages over other options for a range of conditions.
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Acknowledgments |
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Conflict of interest: Research at the National Medical Laser Centre is supported by several commercial companies (including Scotia Quanta Nova, DUSA pharmaceuticals, Miravant/Pharmacia-Upjohn Diomed, Hamamatsu Photonics, and Siemens) and charities (including the Association for International Cancer Research, the Wolfson Foundation, the Stanley Thomas Johnson Foundation, and the Sir Jules Thorn Trust).
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References |
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one world or two?
J Photochem Photobiol
1990;
6:
1-12.
Israeli students are refusing to perform intimate examinations on anaesthetised women without their informed consent.