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US20020133147A1 - Removable tip for laser device - Google Patents

Removable tip for laser device
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Publication number
US20020133147A1
US20020133147A1US10/083,088US8308802AUS2002133147A1US 20020133147 A1US20020133147 A1US 20020133147A1US 8308802 AUS8308802 AUS 8308802AUS 2002133147 A1US2002133147 A1US 2002133147A1
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US
United States
Prior art keywords
laser
skin
laser beam
yag
site
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Abandoned
Application number
US10/083,088
Inventor
Kevin Marchitto
Stephen Flock
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Transmedica International Inc USA
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Transmedica International Inc USA
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Priority claimed from US08/126,241external-prioritypatent/US5643252A/en
Application filed by Transmedica International Inc USAfiledCriticalTransmedica International Inc USA
Priority to US10/083,088priorityCriticalpatent/US20020133147A1/en
Publication of US20020133147A1publicationCriticalpatent/US20020133147A1/en
Priority to MXPA04006099Aprioritypatent/MXPA04006099A/en
Priority to IL16262902Aprioritypatent/IL162629A0/en
Priority to CNB02828187XAprioritypatent/CN100340205C/en
Priority to HK05109228.0Aprioritypatent/HK1077183B/en
Priority to US10/734,529prioritypatent/US20040127815A1/en
Priority to CL200401542Aprioritypatent/CL2004001542A1/en
Abandonedlegal-statusCriticalCurrent

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Abstract

The present invention provides an improved method of measuring analytes in bodily fluids without the use of a sharp. The method having the steps of irradiating the skin of a patient by focused pulses of electromagnetic energy emitted by a laser. By proper selection of wavelength, energy fluence, pulse temporal width and irradiation spot size, the pulses precisely irradiate the skin to a selectable depth, without causing clinically relevant damage to healthy portions of the skin. After irradiation, interstitial fluid is collected into a container or left on the skin. The interstitial fluid is then tested for a desired analyte to approximate the analyte concentration in other bodily fluids. Alternatively, after the forced formation of a microblister, the epidermis covering the microblister is lysed and the interstitial fluid is subsequently collected and tested.

Description

Claims (72)

We claim:
1. A method of measuring analyte concentrations in bodily fluids, comprising the steps of:
a) focusing a laser beam with sufficient energy fluence to ablate the skin at least as deep as the stratum corneum, but not as deep as the capillary layer;
b) firing the laser to create a site of ablation, the site having a diameter of between 0.5 microns and 5.0 cm;
c) collecting a sample of interstitial fluid released by steps (a) and (b); and
d) testing the interstitial fluid for analyte concentration.
2. The method ofclaim 1 wherein the laser beam has a wavelength of 0.2-10 microns.
3. The method ofclaim 1 wherein the laser beam has a wavelength of between 1.5-3.0 microns.
4. The method ofclaim 1 wherein the laser beam has a wavelength of about 2.94 microns.
5. The method ofclaim 1 wherein the laser beam is emitted by a laser selected from the group consisting of Er: YAG, pulsed CO2, Ho:YAG, Er:YAP, Er/Cr:YSGG, Ho:YSGG, Er:GGSG, Er:YLF, Tm:YAG, Ho:YAG, Ho/Nd:Yalo3, cobalt:MgF2, HF chemical, DF chemical, carbon monoxide, deep UV lasers, and frequency tripled Nd:YAG lasers.
6. The method ofclaim 1 wherein the laser beam is emitted by an Er:YAG laser.
7. The method ofclaim 1 wherein the laser beam-is emitted by a modulated laser selected from the group consisting of continuous-wave CO2, Nd:YAG, Thallium:YAG and diode lasers.
8. The method ofclaim 1 wherein the laser beam is focused at a site on the skin with a diameter of 0.1-5.0 mm.
9. The method ofclaim 1 wherein the energy fluence of the laser beam at the skin is 0.03-100,000 J/cm2.
10. The method ofclaim 1 wherein the energy fluence of the laser beam at the skin is 0.03-9.6 J/cm2.
11. The method ofclaim 1 wherein multiple ablations are made to prepare the skin for diffusion of interstitial fluid.
12. The method ofclaim 1 wherein multiple ablations are made to prepare the skin for pharmaceutical delivery.
13. The method ofclaim 1 further comprising a beam splitter positioned to create, simultaneously from the laser, multiple sites of ablation.
14. The method ofclaim 13 wherein the beam splitter is selected from a series of partially silvered mirrors, a series of dichroic mirrors, and a series of beam-splitting prisms.
15. The method ofclaim 1 further comprising an acousto-optic modulator outside the laser cavity wherein the modulator consecutively deflects the beam at different angles to create different sites of ablation on the skin.
16. The method ofclaim 1 wherein the analyte to be measured is selected from the group consisting of Na+, K+, Ca++, Mg++, Cl, HCO3, HHCO3, phosphates, S4, glucose, amino acid, cholesterol, phospholipids, neutral fat, PO2, pH, organic acids or proteins.
17. The method ofclaim 1 wherein the analyte measurement is used to represent the analyte concentration in blood.
18. The method ofclaim 1 wherein the interstitial fluid is collected in a container positioned proximal to the ablation site and through which the laser beam passes.
19. The method ofclaim 18 wherein the testing of analyte concentration is conducted while the container unit is attached to the laser device.
20. The method ofclaim 1 further comprising the step of applying a therapeutically effective amount of a pharmaceutical composition at the site of ablation.
21. The method ofclaim 20 wherein the pharmaceutical substance is administered based on analyte concentration in the interstitial fluid.
22. The method ofclaim 1 further comprising the step of applying a pressure gradient to the skin after formation of the site of ablation to increase the diffusion rate of interstitial fluid.
23. The method ofclaim 1 further comprising the step of mechanically increasing the diffusion rate of interstitial fluid after formation of a site of ablation.
24. The method ofclaim 23 wherein diffusion is increased by the application of subatmospheric pressure at the ablation site.
25. The method ofclaim 24 wherein the container unit is under subatmospheric pressure
26. The method ofclaim 1 wherein a pressure gradient is created at the site of ablation to increase the removal of bodily fluids.
27. A method of measuring analyte concentrations in bodily fluids, comprising the steps of:
a) focusing a laser beam with sufficient energy fluence to alter the skin at least as deep as the stratum corneum, but not as deep as the capillary layer; and
b) firing the laser to create a site of alteration, the site having a diameter of between 0.5 microns and 5.0 cm.
c) collecting a sample of interstitial fluid released by steps (a) and (b); and
d) testing the fluid for analyte concentration.
28. The method ofclaim 27 wherein the laser beam has a wavelength of 0.2-10 microns.
29. The method ofclaim 27 wherein the laser beam has a wavelength of between 1.5-3.0 microns.
30. The method ofclaim 27 wherein the laser beam has a wavelength of about 2.94 microns.
31. The method ofclaim 27 wherein the laser beam is emitted by a laser selected from the group consisting of Er:YAG, pulsed CO2, Ho:YAG, Er:YAP, Er/Cr:YSGG, Ho:YSGG, Er:GGSG, Er:YLF, Tm:YAG, Ho:YAG, Ho/Nd:Yalo3, cobalt:MgF2, HF chemical, DF chemical, carbon monoxide, deep UV lasers, and frequency tripled Nd:YAG lasers.
32. The method ofclaim 27 wherein the laser beam is emitted by an Er:YAG laser.
33. The method ofclaim 27 wherein the laser beam is emitted by a modulated laser selected from the group consisting of continuous-wave CO2, Nd:YAG, Thallium:YAG and diode lasers.
34. The method ofclaim 27 wherein the laser beam is focused at a site on the skin with a diameter of 0.1-5.0 mm.
35. The method ofclaim 27 wherein the energy fluence of the laser beam at the skin is 0.03-100,000 J/cm2
36. The method ofclaim 27 wherein the energy fluence of the laser beam at the skin is 0.03-9.6 J/cm2.
37. The method ofclaim 27 wherein multiple alterations are made to prepare the skin for diffusion of interstitial fluid.
38. The method ofclaim 27 wherein multiple alterations are made to prepare the skin for pharmaceutical delivery.
39. The method ofclaim 27 further comprising a beam splitter positioned to create, simultaneously from the laser, multiple sites of alteration.
40. The method ofclaim 39 wherein the beam splitter is selected from a series of partially silvered mirrors, a series of dichroic mirrors, and a series of beam-splitting prisms.
41. The method ofclaim 27 further comprising an acousto-optic modulator outside the laser cavity wherein the modulator consecutively deflects the beam at different angles to create different sites of alteration on the skin.
42. The method ofclaim 27 wherein the analyte to be measured is selected from the group consisting of Na+, K+, Ca++, Mg++, Cl, HCO3, HHCO3, phosphates, S4, glucose, amino acid, cholesterol, phospholipids, neutral fat, PO2, pH, organic acids or proteins.
43. The method ofclaim 27 wherein the analyte measurement is used to represent the analyte concentration in blood.
44. The method ofclaim 27 wherein the interstitial fluid is collected in a container positioned proximal to the ablation site and through which the laser beam passes.
45. The method ofclaim 27 wherein the testing of analyte concentration is conducted while the container unit is attached to the laser device.
46. The method ofclaim 27 further comprising the step of applying a therapeutically effective amount of a pharmaceutical composition at the site of alteration.
47. The method ofclaim 46 wherein the pharmaceutical substance is administered based on analyte concentration in the interstitial fluids.
48. The method ofclaim 27 further comprising the step of applying a pressure gradient to the skin after formation of the site of ablation to increase the diffusion rate of interstitial fluid.
49. The method ofclaim 27 further comprising the step of mechanically increasing the diffusion rate of interstitial fluid after formation of a site of alteration.
50. The method ofclaim 49 wherein diffusion is increased by the application of sub-atmospheric pressure at the alteration site.
51. The method ofclaim 50 wherein the container unit is under sub-atmospheric pressure.
52. The method ofclaim 27 wherein a pressure gradient is created at the site of alteration to increase the removal of bodily fluids.
53. A method of measuring analyte concentration in bodily fluids, comprising the steps of:
a) applying sub-atmospheric pressure at the surface of the skin to induce the formation of a microblister;
b) focusing a laser beam with sufficient energy fluence to lyse a microblister;
c) firing the laser to lyse the blister;
d) collecting a sample of interstitial fluid released by steps (a), (b) and (c); and
e) testing the fluid for analyte concentration.
54. The method ofclaim 53 wherein the laser beam has a wavelength of 0.2-10 microns.
55. The method ofclaim 53 wherein the laser beam has a wavelength of between 1.5-3.0 microns.
56. The method ofclaim 53 wherein the laser beam has a wavelength of about 2.94 microns.
57. The method ofclaim 53 wherein the laser beam is emitted by a laser selected from the group consisting of Er:YAG, pulsed CO2Ho:YAG, Er:YAP, Er/Cr:YSGG, Ho:YSGG, Er:GGSG, Er:YLF, Tm:YAG, Ho:YAG, Ho/Nd:Yalo3, cobalt:MgF2, HF chemical, DF chemical, carbon monoxide, deep UV lasers, and frequency tripled Nd:YAG lasers.
58. The method ofclaim 53 wherein the laser beam is emitted by an Er:YAG laser.
59. The method ofclaim 53 wherein the laser beam is emitted by a modulated laser selected from the group consisting of continuous-wave CO2, Nd:YAG, Thallium:YAG and diode lasers.
60. The method ofclaim 53 wherein the laser beam is focused at a site on the skin with a diameter of 0.1-5.0 mm.
61. The method ofclaim 53 wherein the energy fluence of the laser beam at the skin is 0.03-100,000 J/cm2.
62. The method ofclaim 53 wherein the energy fluence of the laser beam at the skin is 0.03-9.6 J/cm2.
63. The method ofclaim 53 wherein multiple microblisters are made for collection of interstitial fluid.
64. The method ofclaim 53 further comprising a beam splitter positioned to lyse, simultaneously from the laser, multiple microblisters.
65. The method ofclaim 64 wherein the beam splitter is selected from a series of partially silvered mirrors, a series of dichroic mirrors, and a series of beam-splitting prisms.
66. The method ofclaim 53 further comprising an acousto-optic modulator outside the laser cavity wherein the modulator consecutively deflects the beam at different angles to lyse different microblisters.
67. The method ofclaim 53 wherein the analyte to be measured is selected from the group consisting of Na+, K+, Ca++, Mg++, Cl, HCO3, HHCO3, phosphates, S4, glucose, amino acid, cholesterol, phospholipids, neutral fat, PO2, pH, organic acids or proteins.
68. The method ofclaim 53 wherein the analyte measurement is used to represent the analyte concentration in blood.
69. The method ofclaim 53 wherein the interstitial fluid is collected in a container positioned proximal to the microblister and through which the laser beam passes.
70. The method ofclaim 53 wherein the testing of analyte concentration is conducted while the container unit is attached to the laser device.
71. The method ofclaim 53 further comprising the step of applying a therapeutically effective amount of a pharmaceutical composition at the site of the lysed microblister.
72. The method of claim71 wherein the pharmaceutical substance is administered based on analyte concentration in the interstitial fluid.
US10/083,0881993-09-242002-02-26Removable tip for laser deviceAbandonedUS20020133147A1 (en)

Priority Applications (7)

Application NumberPriority DateFiling DateTitle
US10/083,088US20020133147A1 (en)1993-09-242002-02-26Removable tip for laser device
MXPA04006099AMXPA04006099A (en)2001-12-182002-12-13Method and apparatus for treatment of mono-frequency tinnitus.
IL16262902AIL162629A0 (en)2001-12-182002-12-13Method and apparatus for treatment of mono-frequency tinnitus
CNB02828187XACN100340205C (en)2001-12-182002-12-13 Device and method for treating single frequency tinnitus
HK05109228.0AHK1077183B (en)2001-12-182002-12-13Method and apparatus for treatment of mono-frequency tinnitus
US10/734,529US20040127815A1 (en)1993-09-242003-12-11Removable tip for laser device
CL200401542ACL2004001542A1 (en)2001-12-182004-06-21 METHOD FOR TREATING PATIENTS WITH TINNITUS THAT INCLUDES: a) ENABLING EACH PATIENT TO DETERMINE HIS TONE OF TINNITUS; B) APPLY TO THE PATIENT AN EXTERNALLY GENERATED SOUND WAVE; AND C) SCROLL SUCH SOUND WAVE GENERATED EXTERNALLY A

Applications Claiming Priority (5)

Application NumberPriority DateFiling DateTitle
US08/126,241US5643252A (en)1992-10-281993-09-24Laser perforator
US79233597A1997-01-311997-01-31
US08/955,982US6056738A (en)1997-01-311997-10-22Interstitial fluid monitoring
US09/443,782US6387059B1 (en)1993-09-241999-11-19Interstitial fluid monitoring
US10/083,088US20020133147A1 (en)1993-09-242002-02-26Removable tip for laser device

Related Parent Applications (1)

Application NumberTitlePriority DateFiling Date
US09/443,782ContinuationUS6387059B1 (en)1993-09-241999-11-19Interstitial fluid monitoring

Related Child Applications (1)

Application NumberTitlePriority DateFiling Date
US10/734,529ContinuationUS20040127815A1 (en)1993-09-242003-12-11Removable tip for laser device

Publications (1)

Publication NumberPublication Date
US20020133147A1true US20020133147A1 (en)2002-09-19

Family

ID=25156545

Family Applications (13)

Application NumberTitlePriority DateFiling Date
US08/955,789Expired - Fee RelatedUS6315772B1 (en)1992-10-281997-10-22Laser assisted pharmaceutical delivery and fluid removal
US08/955,982Expired - Fee RelatedUS6056738A (en)1993-09-241997-10-22Interstitial fluid monitoring
US08/955,545Expired - Fee RelatedUS6251100B1 (en)1993-09-241997-10-22Laser assisted topical anesthetic permeation
US09/443,782Expired - Fee RelatedUS6387059B1 (en)1993-09-241999-11-19Interstitial fluid monitoring
US09/457,953Expired - Fee RelatedUS6443945B1 (en)1992-10-281999-12-09Laser assisted pharmaceutical delivery and fluid removal
US09/589,865Expired - Fee RelatedUS6419642B1 (en)1993-09-242000-06-08Irradiation enhanced permeation and delivery
US09/590,150Expired - Fee RelatedUS6425873B1 (en)1993-09-242000-06-08Irradiation enhanced permeation and collection
US10/083,088AbandonedUS20020133147A1 (en)1993-09-242002-02-26Removable tip for laser device
US10/091,957AbandonedUS20030045867A1 (en)1993-09-242002-03-05Removable tip for laser device with safety interlock
US10/098,909AbandonedUS20030097123A1 (en)1992-10-282002-03-13Removable tip for laser device with transparent lens
US10/734,529AbandonedUS20040127815A1 (en)1993-09-242003-12-11Removable tip for laser device
US10/747,988AbandonedUS20040143248A1 (en)1993-09-242003-12-29Removable tip for laser device with safety interlock
US10/831,641AbandonedUS20050010198A1 (en)1992-10-282004-04-23Removable tip for laser device with transparent lens

Family Applications Before (7)

Application NumberTitlePriority DateFiling Date
US08/955,789Expired - Fee RelatedUS6315772B1 (en)1992-10-281997-10-22Laser assisted pharmaceutical delivery and fluid removal
US08/955,982Expired - Fee RelatedUS6056738A (en)1993-09-241997-10-22Interstitial fluid monitoring
US08/955,545Expired - Fee RelatedUS6251100B1 (en)1993-09-241997-10-22Laser assisted topical anesthetic permeation
US09/443,782Expired - Fee RelatedUS6387059B1 (en)1993-09-241999-11-19Interstitial fluid monitoring
US09/457,953Expired - Fee RelatedUS6443945B1 (en)1992-10-281999-12-09Laser assisted pharmaceutical delivery and fluid removal
US09/589,865Expired - Fee RelatedUS6419642B1 (en)1993-09-242000-06-08Irradiation enhanced permeation and delivery
US09/590,150Expired - Fee RelatedUS6425873B1 (en)1993-09-242000-06-08Irradiation enhanced permeation and collection

Family Applications After (5)

Application NumberTitlePriority DateFiling Date
US10/091,957AbandonedUS20030045867A1 (en)1993-09-242002-03-05Removable tip for laser device with safety interlock
US10/098,909AbandonedUS20030097123A1 (en)1992-10-282002-03-13Removable tip for laser device with transparent lens
US10/734,529AbandonedUS20040127815A1 (en)1993-09-242003-12-11Removable tip for laser device
US10/747,988AbandonedUS20040143248A1 (en)1993-09-242003-12-29Removable tip for laser device with safety interlock
US10/831,641AbandonedUS20050010198A1 (en)1992-10-282004-04-23Removable tip for laser device with transparent lens

Country Status (11)

CountryLink
US (13)US6315772B1 (en)
EP (2)EP1006902A1 (en)
JP (1)JP2001511668A (en)
CN (1)CN1191793C (en)
AU (1)AU738597B2 (en)
BR (1)BR9807816A (en)
CA (1)CA2282635A1 (en)
EA (1)EA002812B1 (en)
IL (1)IL131189A (en)
NZ (1)NZ337293A (en)
WO (1)WO1998033444A1 (en)

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EA199900695A1 (en)2000-04-24
CN1251508A (en)2000-04-26
BR9807816A (en)2000-03-08
EP1006902A1 (en)2000-06-14
US6425873B1 (en)2002-07-30
US6251100B1 (en)2001-06-26
US6443945B1 (en)2002-09-03
WO1998033444A1 (en)1998-08-06
CA2282635A1 (en)1998-08-06
EP1281367A2 (en)2003-02-05
NZ337293A (en)2002-07-26
EP1281367A3 (en)2006-02-01
CN1191793C (en)2005-03-09
US6419642B1 (en)2002-07-16
IL131189A0 (en)2001-01-28
EA002812B1 (en)2002-10-31
US20030045867A1 (en)2003-03-06
US20040143248A1 (en)2004-07-22
US6056738A (en)2000-05-02
IL131189A (en)2005-11-20
AU5917398A (en)1998-08-25
AU738597B2 (en)2001-09-20
US6387059B1 (en)2002-05-14
JP2001511668A (en)2001-08-14
US6315772B1 (en)2001-11-13
US20050010198A1 (en)2005-01-13
US20030097123A1 (en)2003-05-22
US20040127815A1 (en)2004-07-01

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