Possible light treatment device for Covid 19 and
other lower respiratory diseases.
One of the known respiratory problems associated with COVID-19 is that
their spikes attach to ACE2 enzymes of type 2 pneumocytes in alveolar
epithelium. Type 2 pneumocytes are defenders of the alveolus and synthesize,
secrete and recycle all components of the surfactant that regulates alveolar
surface tension in the lungs. Binding of COVID-19 spike protein to ACE2
down-regulates the enzyme, which contributes to ARDS for unopposed, detrimental
action of ACE on lung tissue, triggering vasoconstriction, inflammation,
apoptosis and fibrosis.
Space limitations:
SARS-CoV-2 virion = (0.1 or 0.065) micron in diameter.
SARS-CoV-2 virion = (0.1 or 0.065) micron in diameter.
1 mm = 1,000 microns
1 micron = 1,000 nm
1 nm = 100 angstroms
1 micron = 1,000 nm
1 nm = 100 angstroms
The average trachea for women is about 20 mm in diameter.
Rt Bronchial between 4 and 7 mm in diameter.
Lt Bronchial between 4 and 6 mm in diameter.
Most small airways are 1 mm to 0.5 mm in diameter, for avg internal diameter of 0.76 mm.
Lung with 5 liter volume contains about 30,000 small airways.
Bronchiole air passages < 1 mm in diameter.
Rt Bronchial between 4 and 7 mm in diameter.
Lt Bronchial between 4 and 6 mm in diameter.
Most small airways are 1 mm to 0.5 mm in diameter, for avg internal diameter of 0.76 mm.
Lung with 5 liter volume contains about 30,000 small airways.
Bronchiole air passages < 1 mm in diameter.
General performance specs for UV thru near IR light treatment device for
lower respiratory tract:
Device to be about 1 meter long, sealed,
flexible, hollow carbon fiber, or possibly PET or PvB tapered tube of 0.4 mm inner diameter and 0.6 mm
outer diameter (smaller if possible) at tip, and about 5 mm inner diameter and 5.2
mm outer diameter at base. Dimensions subject to fit within lungs and dimension needed for wiring of individual steering strands. Number of steering strands may be reduced if needed to fit conductors within device interior space. Outer membrane to be both flexible and slippery, that can
be reused after thorough wash with soap and water, UV or ozone disinfection. Possibly coated with synthetic mucus. Length of tube as required
to extend throughout lower respiratory tract. Outer membrane sealed against
leaks, does not out-gas, does not stain, and can be lightly rubbed against the cilia,
bronchial and lung membranes without damaging them. Tube is mechanically (computer assisted and
steered) reeled or otherwise projected into and out from patient's bronchial
and perhaps tertiary bronchiole tubes to get as close as possible to individual
alveolar sacs. Overall tube size has to be of the smallest diameter possible to
reach these sacs. Adequate speed of device movement is required for minimizing
duration of individual treatment.
Center of tube has two flexible 8.3-micron
diameter fiber optic cables with minimized cladding and jacket thickness. One
for emitting UV thru near-IR light wavelengths, and other for enlarged viewing of bronchial tissues
beyond tip of probe. Flexible fiber optic rod used to project treatment light
has to be of material that transmits full range of wavelengths intended for
treatment of infected areas, or, if just one particular wavelength is
determined most effective, then that particular wavelength. Other flexible
fiber optic rod transmits video view of bronchial and lung spaces and tissues
ahead of probe back to computer programs and monitor on mobile base of device.
Rounded tip of probe is transparent hemispherical plastic. Tube tip
has an adjustable lens for treatment fiber optic rod, to focus treatment light
either into a spot or to spread light out over broad area as selected for
best treatment. Unless acceptable image can be provided via other technology,
such as simultaneous external MRI or CT scan, at probe tip viewing fiber optic
cable has adjustable lens and f-stop to adjust depth of field for needed
clarity of vision of treatment areas.
But both treatment and imaging lenses are kept
clean of debris and mucus to maintain proper operation. Tube has two vessels,
one 15-micron flexible vessel for warmed liquid transport, the other 15-micron
vessel for air, with valves at probe tip. Nozzles sealed to probe tip outer
wall. Vessels adjacent to two central flexible optical cables. First vessel
contains one of: surface applied muscle relaxant or whatever is recommended for
reducing irritation and distress to patients due to intubation; therapeutic
alveolar replacement surfactant similar to that given to preemies; and
liquefied ACE2 enzymes to cause SARS-CoV-2 virion spikes to attach to, to
reduce odds of their attachment to the ACE2 enzymes of the type 2 pneumocytes. Second
vessel is used to vacuum excessive fluid out of alveolar sacs, or to introduce
drying gasses to dry those liquid filled alveolar sacs.
Surrounding the central fiber optic cables and
liquid and gas vessels, near the exterior tube wall are nine equally spaced 2-micron
diameter carbon nanotube steering strands that run parallel to the length of
the tube. Steering strands are used to induce angles into the tube to allow the
tube to be steered into different bronchial subdivisions, and to reduce tube
contact pressure with bronchi. Steering strands are sequentially contracted to
maintain equivalent angles to those of the bronchi structure through which the
device passes. Strands are made from carbon nanotubes which are can be easily
stretched, but can also be reduced in length or contracted via small electric
currents. Watertight connections are made to the ends of the steering strands
at perpendicular frames to which the nanotubes connect. Insulated electric
current leads return to the outside start of the tube near the computer
controller and mobile stand.
Steering strands connect to perpendicular frames spaced
along length of tube. Frames attached to inner surface of tube wall. Spacing of
frames determined by diameter of tube, at about 2 to 3 times diameter of tube
at frame location, unless another spacing is found to be better suited for achieving
appropriate angles necessary for the steering of the tube into patients' bronchi
by alternative location testing.
One negative lead from one side of each
perpendicular frame and the positive lead from each strand are connected to a
switching center. This switching center is controlled by a computer program
designed to keep the steering and angling of the tube synchronized with the
depth of tube feed. In addition to that part of the software program, another
part simultaneously controls the motion of the tube into and out from each individual
bronchus. Another subroutine of the device’s software program controls therapeutic
light frequencies, determined from invitro testing, and that the light is accurately
applied to infecting virions without damaging substrate tissues and immune
system cells and molecules. Another program subroutine controls application of
muscle relaxant during intubation. Separate program subroutine controls
deposition of liquefied enzymes. Yet another program subroutine controls vacuum
or drying gas treatment. Opening of valves, control of focusing lenses and
actuating of pumps within the reservoirs filled with therapeutic liquids and
gasses, are controlled by the device’s software control programs.
Combined projection/retraction, steering and
angling portion of the device’s computer control software program is similar to
that used to autonomously drive cars. Prior or simultaneous X-ray, CT or MRI
patient data is used in conjunction with views from the probe tip to steer the
tube efficiently first to those areas in greatest need of the therapy provided
by the device, and then as a preventative to the secondary nearby alveolar
sacs. Prior investigative data is also used to program location of areas where
prophylactic enzyme deposition is applied, and where alveolar vacuum or drying
gas treatment is applied.
To help computer program better control location
of tube, soft contact of tube wall with bronchial tissue might be used. Tube
might use sinusoidal wave motion (like sidewinder snake motion) and light
contact between tube device and bronchi during intubation to maintain centering
of the tube within the bronchi yet only exert slight pressure on the surrounding
tissues rather than to slide over and rub against or abrade them.
I would hope that such a device could be
automatically controlled by computer software without a great deal of hospital staff
oversight, as the feedback gained from the use of the device would gradually
improve the therapeutic efficacy of the device.