Biopsy device with aperture orientation and improved tip

Information

  • Patent Grant
  • 10105125
  • Patent Number
    10,105,125
  • Date Filed
    Wednesday, January 23, 2013
    11 years ago
  • Date Issued
    Tuesday, October 23, 2018
    6 years ago
Abstract
A biopsy device includes an elongated probe having a central longitudinal axis, a proximal end, a distal end, and an aperture. A tissue penetrating tip includes a proximal base secured to the distal end of the probe. A sharp distal point distal to the proximal base lies on the central longitudinal axis. Each of a first, second and third concave surface is configured to extend from the base to the sharp distal point. The second concave surface is located to intersect the first concave surface to form a first curved cutting edge. A third concave surface is located to intersect the first concave surface to form a second curved cutting edge and is located to intersect the second concave surface to form a third curved cutting edge. Each curved cutting edge extends from the base to the sharp distal point. A tissue cutting device is coaxial with the probe.
Description
FIELD OF THE INVENTION

The present invention relates generally to tissue removing devices such as biopsy devices and the methods of using such devices. More specifically, it is directed to an improved device and method for accessing and removing pathologically suspect tissue from within a patient's body.


BACKGROUND OF THE INVENTION

In diagnosing and treating certain medical conditions, such as potentially cancerous tumors, it is usually desirable to perform a biopsy, in which a specimen of the suspicious tissue is removed for pathological examination and analysis. In many instances, the suspicious tissue is located in a subcutaneous site, such as inside a human breast. To minimize surgical intrusion into the patient's body, it is desirable to be able to insert a small instrument into the patient's body to access the targeted site and to extract the biopsy specimen therefrom.


Electrosurgical techniques have been used in a variety of biopsy procedures. In electrosurgery, high frequency electrical energy is typically applied to patient tissue through an active electrode, the electrical circuit being completed by a return electrode in contact with the patent's tissue. Electrical energy flowing through the tissue from the active electrode is effective to ablate tissue near the active electrode, forming an opening in the tissue and so allowing insertion of the instrument into a patient's body. A return electrode may be placed on the exterior of the patient's body or may be incorporated into the device itself. The return electrode is typically attached to the patient at a point remote from where the primary or active electrode contacts the tissue. However, in the case of a bipolar electrode for example, the return electrode may be disposed near to the active electrode. An electrosurgical biopsy instrument is disclosed and claimed in U.S. patent application Ser. No. 09/159,467 for “Electrosurgical Biopsy Device and Method,” now U.S. Pat. No. 6,261,241, assigned to the assignee of the present application, and which is hereby incorporated by reference in its entirety. A variety of needle like tip designs have been developed to aid in the accessing of intracorporeal sites for biopsy and other procedures. Electrosurgical techniques have also been used in a variety of biopsy procedures to gain access to an intracorporeal site. See for example U.S. Pat. No. 6,261,241, assigned to the assignee of the present application, and which is hereby incorporated by reference in its entirety.


The prior needle like tips do not always allow proper placement of the biopsy or other surgical device. Moreover, while the electrosurgical biopsy devices have been found to be effective in many instances, they are not suitable for use in conjunction with magnetic resonance imaging.


While these electrosurgical biopsy devices have been found to be effective in many instances, they may not always be suitable for use in conjunction with magnetic resonance imaging.


SUMMARY OF THE INVENTION

This invention is directed to devices for accessing and severing tissue from a target site within a patient and methods for utilizing such devices. The devices embodying features of the invention provide access to a targeted tissue site within a patient and provide for the selection, separation and capture of a tissue specimen from supporting tissue at the targeted site.


A tissue accessing and severing device and system having features of the invention generally include an elongated, preferably disposable probe component having a plurality of operative elements and a driver component configured to receive the elongated probe component and drive the various operative elements of the probe component.


The elongated probe component has a distal shaft portion with a tissue penetrating distal tip, a tubular section proximal to the distal tip, an inner lumen extending within the tubular section and an open, tissue receiving aperture in the tubular section which provides access to tissue at the targeted site. The probe component includes an elongated tissue-cutting member, which is preferably at least in part cylindrically shaped. The tissue cutting member is provided with at least one tissue cutting edge which is configured to sever tissue extending into the interior of the tubular section through the aperture thereof. The cutting edge on the tissue cutting member may be configured for longitudinal cutting movement and may include oscillating rotational motion and/or reciprocating longitudinal motion to sever specimen tissue extending through the aperture from supporting tissue at the targeted site. The cutting surfaces or edges are radially spaced from a longitudinal axis of the probe component and are generally transversely oriented with respect to the longitudinal axis. The tissue cutter is preferably slidably disposed within the inner lumen of the tubular section, although it may be disposed about the tubular section. The probe component may also have a handle which releasably engages the driver component.


In one embodiment of the invention, the cutting member has an inner lumen preferably extending to the proximal end thereof for tissue specimen removal. While mechanical withdrawal of the tissue specimen may be employed, it is preferred to provide a vacuum within the cutting member from the proximal end of the cutting member. The proximal end of the cutting member may be configured to be in fluid communication with a vacuum source to aspirate the severed tissue specimen through the inner lumen of the cutting member to a tissue collection station. A higher fluid pressure may be maintained in the inner lumen of the cutting member distal to the tissue specimen to aid in transporting the specimen proximally through the inner lumen. In this manner, the mechanical withdrawal and/or the vacuum on the proximal end of the specimen and a higher pressure on the distal end of the specimen can move the specimen through the inner lumen of the cutting member to a tissue collection station.


In at least one embodiment, the handle of the probe component is secured, preferably releasably secured, to the driver housing provided to operably connect the various operative elements of the probe with operative elements of the driver component. The tissue cutting member is operatively connected to at least one driver to provide the desired cutting motion. The proximal end of the tubular section is rotatably secured within the handle housing so that the orientation thereof with respect to the longitudinal axis and therefore the orientation of the tissue receiving aperture within the tubular section, can be selected. The orientation of the aperture may be selected manually such as described in copending application Ser. No. 10/642,406, filed February Aug. 15, 2003 or it may be preset or selected electronically by a control module which also controls the operation of the cutting member and electrical power. The aperture orientation setting may be selected before or after the distal portion of the probe component is inserted into the patient.


The tissue penetrating distal tip embodying features of the invention has a proximal base secured to the distal end of the probe shaft of the biopsy device, and a sharp distal point distal to the proximal base. The tissue penetrating distal tip has a first concave surface extending from the base to the sharp distal point. The distal tip also has a second concave surface, which intersects the first concave surface forming therewith a first curved cutting edge that leads to the sharp distal point. The distal tip also has a third concave surface which intersects the first concave surface forming therewith a second curved cutting edge leading to the sharp distal point and also intersects the second concave surface forming therewith a third curved cutting edge that leads to the sharp distal point. The concave surfaces preferably have center lines which extend from the proximal base of the distal tip to the sharp distal point. In a presently preferred embodiment the concave surfaces are of the same area. However, they may have different areas.


The driver component has at least two and preferably three driver units for operating the probe component secured to the driver component. Specifically, the driver component has a first driver unit for rotating the tubular section of the probe component, a second driver unit for moving the cutting member along a longitudinal axis of the cutting member and optionally a third driving unit for rotating or oscillating the cutting member about the longitudinal axis. The first driver unit rotates the tubular section of the probe component, preferably in discrete steps, so that the location of the tissue receiving aperture in the distal extremity of the tubular section can be selected prior to or during the procedure. The discrete rotational steps of the tubular section are preferably in 30° or multiples thereof so that the rotational movement will follow 12 hour clock markings. Preferably, the second and third driver units are operable together so that the cutting member may rotate or oscillate about a longitudinal axis as the cutter member is moved longitudinally. This allows a rotation or an oscillation of the cutter during the cutting process which can aid in cutting tissue.


The driver component may have one or more light sources in a distal portion thereof to illuminate the accessing site during the procedure.


A method of cutting and collecting a tissue specimen with a tissue collection device embodying features of the invention includes advancing such a device at least partially into tissue at a desired site within the patient's body with the tissue penetrating distal tip of the outer cannula disposed distal to the tissue specimen to be separated from the target site. A vacuum is established within the inner lumen of the tubular section to draw tissue through the aperture therein into the inner lumen of the tubular section. The cutting member, which is slidable disposed within the inner lumen of the tubular section, may then be moved longitudinally to cut a tissue specimen from supporting tissue at the target site by the longitudinal motion, which preferably includes oscillating rotational movement and/or reciprocating longitudinal movement. The vacuum established within the inner lumen of the tubular section may be applied through the inner lumen of the tissue cutting member when the tissue cutting member is disposed within the tubular section. The applied vacuum within the inner lumen of the tissue cutting member, may also be utilized to pull or aspirate the separated tissue sample proximally. In addition, or alternatively, a higher fluid pressure may be maintained in a distal part of the inner lumen of the tubular section, distal to the specimen, to push the tissue specimen proximally. Alternatively, the tissue specimen may be mechanically withdrawn. Fluid pressure may include pressure from a liquid delivered into the interior of the device, such as a physiological saline solution, and may include a gas, such as pressurized carbon dioxide, nitrogen or air, delivered into the interior of the device. Access to ambient air can also maintain a sufficiently high pressure differential to move the specimen through the inner lumen of the cutting member. Anesthetic may be injected to the target site through the outer cannula or the inner lumen of the cutting member. Upon removal from the patient, the tissue specimen may then be subjected to pathological examination. After acquisition of a tissue specimen or specimens, the tissue separation system may be repositioned for further tissue separation and collection or it may be withdrawn from the patient.


The tubular section of the probe provides the support for the probe to enable precise location of the accessing port to the desired location at the target site with its radial orientations being preset before the device is introduced into the patient or selected after the tubular section is disposed within the patient. The cutting member quickly and cleanly severs the tissue specimen drawn into the interior of the tubular section though the aperture by the action of the vacuum or otherwise. Upon removal of the tissue specimen, the tissue receiving aperture may be radially repositioned about the longitudinal axis of the tubular section of the probe component so that a plurality of specimens may be taken from the target site. The orientation of the tissue receiving aperture during the procedure may follow a preselected pattern or may be selected by the physician for other selected tissue specimens.


A tissue acquisition system assembly embodying features of the invention may include a device for delivery of one or more marker bodies through a tubular member of a biopsy device such as the tubular cutting member. Such a marker delivery device includes an elongated shaft having an inner lumen and a discharge opening in a distal portion of the elongated shaft, at least one marker body which is disposed within the inner lumen of the elongated shaft, a pusher element which is slidably disposed within the delivery device and which is configured to urge at least one marker body out the discharge opening in the distal portion of the elongated shaft. The marker delivery device has a distally flared guide member which is slidably disposed on the elongated shaft to guide the distal portion of the elongated shaft into a proximal end of the tubular member of a biopsy device. This invention is directed to a tissue penetrating probe tip, particularly for biopsy devices. These devices provide access to a targeted tissue site and provide for the separation and capture of a tissue specimen from supporting tissue at the targeted site.


These and other advantages of the invention will become more apparent from the following detailed description of the invention and the accompanying exemplary drawings.





BRIEF DESCRIPTION OF THE DRAWINGS


FIG. 1 is an exploded view of the elongated tissue biopsy system embodying features of the invention.



FIG. 2 is a perspective view of the embodiment shown in FIG. 1 in an assembled condition without a housing cover for the probe component.



FIG. 3 is a side elevational view of the tissue biopsy device shown in the FIG. 2.



FIG. 4A is a longitudinal cross-section of the probe shown in FIG. 3 taken along the lines 4-4 with the tissue cutting element in a withdrawn position.



FIG. 4B is a longitudinal cross-section of the probe shown in FIG. 3 taken along the lines 4-4 with the tissue cutting element in a forward or closed position.



FIG. 5 is a transverse cross-sectional view of the probe shown in FIG. 4B taken along the lines 5-5.



FIG. 6 is a perspective view of the underside of the probe shown in FIG. 1.



FIG. 7 is an enlarged perspective view of the distal end of the driver unit shown in FIG. 1.



FIG. 8 is an enlarged perspective view of the distal end of the probe housing illustrating a marker element which depicts the orientation of the aperture in the tubular section of the biopsy device.



FIG. 9 is a perspective view of the underside of the driver shown in FIG. 1.



FIG. 10 is an elevational view of a tissue penetrating tip embodying features of the invention.



FIG. 11 is a perspective view of the underside of the tip shown in FIG. 10.



FIG. 12 is a longitudinal, center line cross-sectional view of the penetrating tip shown in FIG. 10.



FIG. 13 is a longitudinal cross-sectional view of the penetrating tip shown in FIG. 12 taken along the lines 13-13.



FIG. 14 is a longitudinal cross-sectional view of the penetrating tip shown in FIG. 12 taken along the lines 14-14.



FIG. 15 is a longitudinal cross-sectional view of the penetrating tip shown in FIG. 3 taken along the lines 15-15.



FIG. 16 is a bottom view of the penetrating tip shown in FIG. 10.



FIG. 17 is a transverse cross-sectional view of the penetrating tip shown in FIG. 16 taken along the lines 17-17.



FIG. 18 is a transverse cross-sectional view of the penetrating tip shown in FIG. 16 taken along the lines 18-18.



FIG. 19 is a transverse cross-sectional view of the penetrating tip shown in FIG. 16 taken along the lines 19-19.



FIG. 20 is a transverse cross-sectional view of the penetrating tip shown in FIG. 16 taken along the lines 20-20.



FIG. 21 is a perspective view of the tissue biopsy system shown in FIG. 1 assembled and mounted on a stereotactic frame.



FIG. 22 is an elevational view of a marker delivery device with a flared guide on the distal end of the shaft which facilitates guiding the distal tip of a marker delivery device into the interior of the proximal end of the tissue cutter.



FIG. 23 is a longitudinal cross-sectional view of the distal end of the marker delivery device and flared guide disposed within the tissue collection component shown in FIG. 1.



FIG. 24 is a longitudinal cross sectional view of the proximal end of the marker delivery device with the flared guide at the proximal end of the shaft and with the shaft deployed within the inner lumen of the tissue cutter.





DETAILED DESCRIPTION OF EMBODIMENTS OF THE INVENTION


FIGS. 1-3 illustrate a biopsy system 10 embodying features of the invention which includes a disposable probe component 11, a driver component 12 and specimen collector 13.


The probe component 11 generally includes an elongated distal shaft 14 having a tubular section or cannula 15 with a tissue penetrating tip 16 on the distal end thereof and an open, tissue receiving aperture 17. The probe component 11 also includes a probe housing 18 with a housing cover 19 which is configured to interfit with the driver component 12. A tissue cutter 20 is slidably disposed within the probe and has a distal cutting surface 21 which severs tissue which extends through the tissue receiving aperture 17.


Details of the probe component 11 are further shown in FIGS. 4A and 4B. The probe housing 18 has a mechanical system for rotating the housing and the tubular section 15 secured thereto to control the angular position of the tissue receiving aperture 17 and for moving the tissue cutter 20 slidably disposed within the probe component 11.


The mechanical system of the driver component 12 has first driving gear 22 that is configured to engage the probe gear 23 and rotate the probe housing 18 so as to adjust the orientation of aperture 17 in the distal extremity of the tubular section 15. The probe gear 23 is secured to the rotating connector body 24 by adhesive 25. The proximal extremity of the tubular section 15 is secured to the rotating connector body 24 by adhesive 26. An end cap 27 retains the connector body 24 within the probe housing 18. Rotation of the probe gear 23 rotates the connector body 24 and the attached tubular section 15. The rotation is preferably controlled so that the tubular section 15 rotates in discrete steps about the longitudinal axis 28 to adjust the angular orientation of the aperture 17 about the longitudinal axis. Preferably these discrete orientations may be provided in increments of 30° which can be readily indicated by arrow 29 at the distal end of the probe housing 18 as shown in FIG. 8.


The second driving gear 30 is configured to drive the tissue cutter 20 longitudinally. The driving gear 30 engages probe gear 31 which drives cutter traverse nut 32 and cutter screw 33 threadably connected to the cutter traverse nut. The distal end of the cutter screw 33 is provided with a recess 34 which receives the rib 35 of the cutter shuttle 36. The cutter shuttle 36 is secured to the tissue cutter 20 by adhesive 37. The probe gear 31 is secured to the cutter traverse nut 32 by adhesive 38. Rotation of the probe gear 31 adjusts the relative axial position of the cutter screw 33 with respect to the cutter traverse nut 32 which is secured to the cutter shuttle 36. Longitudinal movement of the tissue cutter 20 follows the longitudinal movement of the cutter shuttle 36 resulting from the movement of cutter screw 33. The length of the tissue receiving aperture 17, and as a result the length of the specimen, can be controlled by adjusting the initial longitudinal position of the distal end of the tissue cutter 20 within the aperture, before cutting.


The third driving gear 40 is configured to rotate or oscillate the tissue cutter 20 as the cutter moves along the longitudinal axis 28 to facilitate the cutting action of the cutting surface 21 on the distal end of the cutter. The third driving gear 40 engages probe gear 41 which is secured to cutter oscillation shaft 42 by adhesive 43. The probe gear 41 may be oscillated back and forth about the longitudinal axis 28 or rotated continuously in a single direction about the longitudinal axis, or both depending upon the desired rotational movement of the tissue cutter.


A biased valve assembly 44 is provided in the distal end of the probe housing 18 to ensure sealing when a vacuum is developed within the interior 45 of the tissue cutter 20 while providing an atmospheric vent 46 between the interior surface 47 of the tubular section 15 and the exterior surface 48 of the tissue cutter 20. The valve assembly 44 includes a spring 49, valve body 50 and a valve collar 51 which is secured to the proximal end of the tubular section 15 by adhesive 52. The proximal end of the valve spring 49 rests against the shoulder 53 provided in the exterior of the valve body 50. A biased cutter shaft seal 54 slidably engages the exterior 48 of the tissue cutter 20.


The tissue specimen collector 13 is secured to the proximal end of the housing of probe component 11 and has an interior 55 in fluid communication with the inner lumen 56 extending within the tissue cutter 20 and has a removable proximal wall 57 of specimen receiving cartridge 58 which gives access to the interior 55 and any tissue specimens which may have been drawn therein. A vacuum is generated within the interior 55 to draw tissue specimens through the inner lumen 45 into the interior 55. Tubular member 59 has a distal end which is in fluid communication with the interior 55 of the tissue specimen collector 13 and has a proximal end (not shown) which is configured to be connected to a vacuum source. Application of a vacuum within the tubular member 59 aids in pulling tissue into the interior 17 of the tubular section 15 and transfer of the severed tissue specimen through the inner lumen 45 of the tissue cutter 20 to the specimen cartridge 58.


The driver 12 has a housing 60 with an upper concave surface 61 which is configured to receive the lower surface 62 of the probe housing 18. Three partially exposed driving gears 22, 30 and 40 are provided on the proximal end of the driver 12 which are configured to engage the probe gears 23, 31 and 41 respectively. The drive 12 is provided with three separately operating drive motors (not shown) which drive the drive gears 22, 30 and 40. The separate drive motors (not shown) are connected to and the operation thereof controlled by a control module, such as described in copending application Ser. No. 10/847,699, filed on May 17, 2004. The control module controls the motors which move the individual drive gears 22, 30 and 40. The gear 22 engages gear 23 in the probe 11 to control the rotation of the probe housing 18 and the location and orientation of the tissue receiving aperture 17. The drive gear 30 engages probe gear 31 to control the longitudinal position and motion of the tissue cutter 20 along the longitudinal axis 28. Drive gear 40 engages probe gear 41 to control the oscillation or rotation of the tissue cutter 20 about the longitudinal axis 28.


As shown in FIG. 7, the front face of the driver component 12 is provided with light sources 66 and 67 and a manually activatable switch 68 to activate the light sources and enable the physician and other operating personnel to better view the operating site on the patient. Other manual switches, e.g. a foot activated switch, may be employed. Alternatively, the light sources may be automatically activated when the probe component 11 is installed on the driver 12 or other events such as when electrical power is turned on. The driver component 12 may have a battery pack for the light sources 66 and 67.


The tissue penetrating distal tip 16 may have a variety of tip shapes. A particularly suitable distal tip embodying features of the invention is shown in FIGS. 9-20. The tissue penetrating distal tip generally includes a base 70, a sharp distal point 71, a first concave surface 72, a second concave surface 73 and a third concave surface 74.


The intersection between the first concave surface 72 and the second concave surface 73 forms the first curved cutting edge 75. The intersection between the second concave surface 73 and the third concave surface 74 forms the second curved cutting edge 76. The intersection between the third concave surface and the first concave surface 72 forms the third curved cutting surface 77.


The concave surfaces 72, 73 and 74 are hollow ground and the pentrating tip 16 is then electro-polished to increase the sharpness of the cutting edges 75, 76 and 77. The penetrating distal tip 16 may be formed of suitable surgical stainless steel such as 17-4 stainless steel. Other materials may be suitable. The penetrating distal tip 16 is preferably electro-polished in an acidic solution to sharpen the curved cutting edges and thereby facilitate tissue penetration. Suitable electro-polishing solutions include Electro Glo sold by the Electro Glo Distributing Co.


The base 70 of the tissue penetrating tip 16 may be secured to the distal end of the elongated shaft of the biopsy device 10 for accessing and collecting tissue from a target site within a patient. The sharp distal tip 16 embodying features of the invention readily penetrates a patient's tissue, particularly breast tissue and facilitates guiding the distal end of the biopsy or other device to a desired intracorporeal location.


The tissue penetrating tips may also be employed on biopsy devices such as those described in co-pending application Ser. No. 10/642,406, filed on Aug. 15, 2003, which is assigned to the present assignee. Alternatively, the distal tip may be provided with an arcuate RF electrode such as disclosed in U.S. Pat. No. 6,261,241, and U.S. Pat. No. 6,471,700, both assigned to the present assignee.


The separate driver component 12 allows the probe unit 11 to be disposable. The drive gears of the drive component 12 control the motion of the tissue cutting member 20 for cutting and the motion of the tubular section 15 to orient the aperture 17. Other means (not shown) may provide mechanical and electrical power, vacuum, and control to the probe device. Examples of replaceable snap-in type probe units are disclosed in Burbank et al., U.S. patent application Ser. No. 10/179,933, “Apparatus and Methods for Accessing a Body Site”. Drive units such as that described in WO 02/069808 (which corresponds to co-pending U.S. application Ser. No. 09/707,022, filed Nov. 6, 2000 and U.S. application Ser. No. 09/864,021, filed May 23, 2001), which are assigned to the present assignee, may be readily modified by those skilled in the art to accommodate the movement of the cutting member 20.


In use, the distal end of the probe component 11 is advanced within the patient with the tissue cutter 20 in a forward or closed position (FIG. 4B), until the aperture 17 of the tubular section 15 is located in a desired location for taking a tissue specimen. The tissue cutter 20 is then withdrawn proximally to an open position to open the aperture 17. The withdrawal of the tissue cutter can be used to control the length of the aperture which is opened in order to control the length of the specimen which is severed. A vacuum is applied to the interior 45 of the tissue cutter 20 to draw tissue at the site into the inner lumen of the tubular section 15 through the aperture 17. The tissue cutter 20 is then driven distally by rotation of probe gear 30 and rotated or oscillated by drive gear 40 engaging probe gear 41 to sever the aspirated tissue from the supporting tissue at the target site with the tissue cutting surface 21. The vacuum within the interior of the tissue cutter 20 causes the tissue specimen to be drawn through the inner lumen 45 of the tissue cutter 20 and into the cartridge 58 of specimen collector 13 shown in FIG. 2. Positive pressure or even ambient conditions distal to the tissue specimen can facilitate tissue passing through the interior 45 of tissue cutter 20. If another tissue specimen is desired, the tubular section 15 may be rotated by the drive gear 22 engaging the probe gear 23 in one or more steps to repeat obtaining another tissue specimen in the same manner without otherwise moving the probe component 11. Typically, a first tissue specimen is obtained with the aperture 17 of the probe 11 in the 12 o-clock position, the second at the 3 o-clock position, the third at the 9 o-clock position and the fourth at the 6 o-clock position. The location of the second and third specimens may be reversed. The position of the aperture 17 may be indicated by a marker arrow 29 at the end cap 27 so that the physician or other operating personnel can readily determine what the orientation of the aperture 17 within the patient.


The biopsy system 10 may be hand held for some biopsy procedures or the system may be mounted on a stereotactic mounting stage 80 as shown in FIG. 21. A shoe 81 is slidably mounted to a rail 82 of a Fisher stage. The mounting member 83 is secured to the shoe 81 by a threaded post (not shown) secured to thumbwheel 84. As shown in FIG. 10, the bottom surface 85 of the driver component 12 is configured to conform at least in part to the upper surface of the mounting member 83. The sampling and vacuum switches 86 and 87 respectively on the driver component 12 are actuated by the optional sampling and vacuum actuating elements 88 and 89 on the mounting member 83. Alternatively, sampling and vacuum may be actuated with a foot pedal. As shown in FIG. 22, the driver component has an operator dial 90 which when turned opens a threaded hole 91 for receiving a threaded post (not shown) secured to the thumbwheel 84 and the locating pin holes 92 and 93 which receive the complementary posts (not shown) in the mounting member 83.


As mentioned above, positive pressure or even ambient conditions will aid in passing the severed tissue specimen through the inner lumen 45 of tissue cutter 20 into the cartridge 58 of specimen collector 13. As shown in FIGS. 4A and 4B venting valve can provide ambient pressure behind the tissue specimen in the cutter interior 45 from the interior of the tubular section 15. The valve body 50 is opened for atmospheric venting when the tissue cutter 20 is in the forward position upon the completion of severing the specimen from the tissue site. However, when the tissue cutter 20 is pulled back proximally the valve spring 49 urges the valve body 50 back to a closed position. While the tissue cutter 20 is shown with a tissue cutting surface 21 which is perpendicular to the longitudinal axis 28, the tissue cutting surface may be at an angle or even parallel to the longitudinal axis as described in co-pending application Ser. No. 10/642,406, filed Aug. 15, 2003.


The distal cutting edge 21 of the tissue cutter 20 may initially be located proximal to the aperture 17 to provide a full aperture for receiving tissue or it can be initially located within the aperture 17 in order to control the length of the specimen. The cutting action of tissue cutter 20 preferably continues until the beveled cutting surface 21 has completely traversed the aperture 17 to ensure that the tissue drawn through the aperture is completely severed from supporting tissue at the biopsy site. A vacuum may be applied to aspirate the severed tissue specimen through the inner lumen of the tissue cutter 20 to the cartridge in the specimen collector at the proximal end of the biopsy device. Positive pressure or access to ambient conditions may be provided in the distal end of the tubular section to aid in the specimen transfer.


After the removable wall 57 of the specimen receiving cartridge 58 is removed and the specimens therein removed, it is frequently desirable to deliver one or more markers to the target site from which the specimens have been removed. Such marker delivery devices are shown in co-pending application Ser. No. 10/753,694, filed on Jan. 7, 2004 and co-pending application Ser. No. 10/444,770, filed May 23, 2003. However, the distal ends of these marker delivery devices are very small and they can be difficult to insert into the proximal end of the tissue cutter 20 which is just slightly larger to accommodate the marker delivery shaft.



FIG. 22 illustrates a marker delivery device 100 which is particularly suitable to facilitate the introduction of the distal end of the shaft 101 into the inner lumen 45 of the tissue cutter 20 and the advancement therein. As shown in FIG. 23, to facilitate the insertion of the small diameter distal tip 101 of the marker delivery device 100 into the slightly larger inner lumen 45 of the tubular cutter 20 at its proximal end, the distal tip is preferably provided with an outwardly flared guide 102 which is slidably mounted on the shaft 103 of the marker delivery device 100. The proximal end of the tubular cutter 20, the flared guide 102 and/or the distal tip 101 may be provided with mating guide elements which orient the marker delivery device with the cannula 15 of the biopsy device. To ensure that one or more markers are discharged through the aperture 17 of the biopsy device 10 when the pusher element slidably disposed within the delivery device is urged distally to press at least one marker body out the discharge opening in the distal portion of the elongated shaft of the marker delivery device. As indicated in FIG. 23, the shaft 103 of the marker delivery device 100 is advanced into the inner lumen 45 of the tissue cutter 20 so that the distal end 101 of the marker delivery device 100 is adjacent to the aperture 17 of the cannula 15. Plunger 104 is pressed further into the inner lumen of shaft 103 to eject one or more markers 105 through the aperture 17 in the tubular section 15 before the biopsy device 10 is removed from the patient. The delivery of markers to the target site after specimen removal, while the distal end of the biopsy device is still at the biopsy site, ensures that the markers are properly position at the biopsy site.


While the slidably mounted, flared proximal guide 102 is described with respect to being disposed on the shaft 103 of marker delivery device 101, the flared guide 102 has wide application within a variety of biopsy and other devices where one small diameter tubular member is to be inserted into a slightly larger, but still small diameter second tubular member.


The elongated probe component 11 of the biopsy system 10 has a length of about 3 to about 20 cm, preferably, about 5 to about 13 cm, and more specifically, about 8 to about 9 cm for breast biopsy use. To assist in properly locating the probe 11 during advancement thereof into a patient's body, the distal extremity of the tubular section may be provided with a marker at a desirable location that provide enhanced visualization by eye, by ultrasound, by X-ray, MRI or other imaging or visualization means. Manual palpation may also be employed. An echogenic polymer coating that increases contrast resolution in ultrasound imaging devices (such as ECHOCOAT™ by STS Biopolymers, of Henrietta, N.Y.) is suitable for ultrasonic visualization. Radiopaque markers may be made with, for example, stainless steel, platinum, gold, iridium, tantalum, tungsten, silver, rhodium, nickel, bismuth, other radiopaque metals, alloys and oxides of these metals. In addition, the surfaces of the device in contact with tissue or other components of the device may be provided with a suitable lubricious coating such as a hydrophilic material or a fluoropolymer.


The tubular section and the tissue cutter are preferably formed of a surgical grade stainless steel. However, other high strength materials such as MP35N, other cobalt-chromium alloys, NiTi alloys, ceramics, glasses, and high strength polymeric materials or combinations thereof may be suitable.


A patient's skin usually must be breached in order to gain access to a body site where a tissue specimen is to be obtained. A scalpel or other surgical instrument may be used to make an initial incision in the skin. After the specimens have been taken, the biopsy device may be removed from the patient. The entire device may be removed; however, in some embodiments, the cartridge 58 may be removed from the system 10 and a delivery cannula may be inserted through the inner lumen of the cutter 20 to deliver markers to the biopsy site through the aperture 17. In addition, it will be readily appreciated that other types of instruments may be inserted into the tissue site through the tissue cutter in addition to or in place of the instruments described above. Moreover, therapeutic or diagnostic agents may be delivered through the tissue cutter 20 or the tubular section 15.


While particular forms of the invention have been illustrated and described herein, it will be apparent that various modifications and improvements can be made to the invention. For example, while the various embodiments of the invention have been described herein in terms of a biopsy device, it should be apparent that the devices and methods of utilizing the device may be employed to remove tissue for purposes other than for biopsy, i.e. for treatment or other diagnoses. Additionally, the tissue penetrating distal tip design may be employed on probes for other uses. Other modifications include, for example, a tissue cutter slidably mounted around the tubular section of the probe component rather than within the tubular section. Moreover, individual features of embodiments of the invention may be shown in some drawings and not in others, but those skilled in the art will recognize that individual features of one embodiment of the invention can be combined with any or all the features of another embodiment. Accordingly, it is not intended that the invention be limited to the specific embodiments illustrated.


Terms such a “element”, “member”, “device”, “section”, “portion”, “means”, “step” and words of similar import, when used in the following claims, shall not be construed as invoking the provisions of 35 U.S.C. § 112(6) unless the claims expressly use the term “means” followed by a particular function without specific structure or the term “step” or “steps” followed by a particular function without specific action. All patents and patent applications referred herein are incorporated by reference in their entirety.

Claims
  • 1. A biopsy device, comprising: a. an elongated probe which has a central longitudinal axis, a proximal end, a distal end, and an aperture proximal to the distal end;b. a tissue penetrating tip, including: i. a proximal base secured to the distal end of the elongated probe,ii. a sharp distal point distal to the proximal base that lies on the central longitudinal axis,iii. a first concave surface configured to extend from the proximal base to the sharp distal point,iv. a second concave surface configured to extend from the proximal base to the sharp distal point and located to intersect the first concave surface to form a first curved cutting edge that extends distally from the proximal base to the sharp distal point, and configured such that the first curved cutting edge has an edge curvature that is concave in a direction toward the central longitudinal axis, andv. a third concave surface circumferentially interposed between the first concave surface and the second concave surface, the third concave surface configured to extend from the proximal base to the sharp distal point and located to intersect the first concave surface to form a second curved cutting edge that extends distally from the proximal base to the sharp distal point and the third concave surface located to intersect the second concave surface to form a third curved cutting edge that extends distally from the proximal base to the sharp distal point, and configured such that each of the second curved cutting edge and the third curved cutting edge has an edge curvature that is concave in a direction toward the central longitudinal axis; andc. a tissue cutting device coaxial with the elongated probe.
  • 2. The biopsy device of claim 1, wherein the first concave surface, the second concave surface and the third concave surface are equi-spaced about the central longitudinal axis of the elongated probe.
  • 3. The biopsy device of claim 1, wherein a surface area of each of the first concave surface, the second concave surface and the third concave surface is the same.
  • 4. The biopsy device of claim 1, wherein a surface concavity of each of the first concave surface, the second concave surface and the third concave surface is the same.
  • 5. The biopsy device of claim 1, wherein a length of each of the first curved cutting edge, the second curved cutting edge, and the third curved cutting edge in a direction along the central longitudinal axis is the same.
  • 6. The biopsy device of claim 5, wherein the first curved cutting edge, the second curved cutting edge, and the third curved cutting edge are positioned at equal angular intervals around the central longitudinal axis.
  • 7. A tissue penetrating tip for use in a medical device, comprising: a base;a sharp distal point that extends distally from the base along a central longitudinal axis;a first concave surface configured to extend from the base to the sharp distal point;a second concave surface configured to extend from the base to the sharp distal point and located to intersect the first concave surface to form a first curved cutting edge that extends distally from the base to the sharp distal point, and configured such that the first curved cutting edge has an edge curvature that is concave in a direction toward the central longitudinal axis; anda third concave surface circumferentially interposed between the first concave surface and the second concave surface, the third concave surface configured to extend from the base to the sharp distal point and located to intersect the first concave surface to form a second curved cutting edge that extends distally from the base to the sharp distal point and the third concave surface located to intersect the second concave surface to form a third curved cutting edge that extends distally from the base to the sharp distal point, and configured such that each of the second curved cutting edge and the third curved cutting edge has an edge curvature that is concave in a direction towards the central longitudinal axis.
  • 8. The tissue penetrating tip of claim 7, wherein the first concave surface, the second concave surface and the third concave surface are equi-spaced about the central longitudinal axis of the elongated probe.
  • 9. The tissue penetrating tip of claim 7, wherein a surface area of each of the first concave surface, the second concave surface and the third concave surface is the same.
  • 10. The tissue penetrating tip of claim 7, wherein a surface concavity of each of the first concave surface, the second concave surface and the third concave surface is the same.
  • 11. The tissue penetrating tip of claim 7, wherein a length of each of the first curved cutting edge, the second curved cutting edge, and the third curved cutting edge in a direction along the central longitudinal axis is the same.
  • 12. The tissue penetrating tip of claim 11, wherein the first curved cutting edge, the second curved cutting edge, and the third curved cutting edge are positioned at equal angular intervals around the central longitudinal axis.
  • 13. The biopsy device of claim 1, wherein the proximal base of the tissue penetrating tip extends in an orthogonal direction to the central longitudinal axis of the elongated probe.
RELATED APPLICATIONS

This application is a continuation of application Ser. No. 11/981,024, now U.S. Pat. No. 8,360,990, which is a divisional of application Ser. No. 11/014,413, filed Dec. 16, 2004, now U.S. Pat. No. 9,408,592, and both are incorporated herein in their entirety and from which priority is claimed.

US Referenced Citations (204)
Number Name Date Kind
2032860 Wappler et al. Mar 1936 A
2525329 Wyzenbeek Oct 1950 A
3341417 Sinaiko Sep 1967 A
3788320 Dye Jan 1974 A
3805791 Seuberth et al. Apr 1974 A
3818894 Wichterle et al. Jun 1974 A
3823212 Chvapil Jul 1974 A
3844272 Banko Oct 1974 A
3847153 Weissman Nov 1974 A
3910279 Okada et al. Oct 1975 A
3945375 Banko Mar 1976 A
3955578 Chamness et al. May 1976 A
4007732 Kvavle et al. Feb 1977 A
4172449 LeRoy et al. Oct 1979 A
4197846 Bucalo Apr 1980 A
4202338 Bitrolf May 1980 A
4234048 Rowley Nov 1980 A
4276885 Tickner et al. Jul 1981 A
4294254 Chamness Oct 1981 A
4311143 Komiya Jan 1982 A
4331654 Morris May 1982 A
4362160 Hiltebrandt Dec 1982 A
4503855 Maslanka Mar 1985 A
4545367 Tucci Oct 1985 A
4565200 Cosman Jan 1986 A
4576162 McCorkle Mar 1986 A
4638802 Okada Jan 1987 A
4643187 Okada Feb 1987 A
4647480 Ahmed Mar 1987 A
4666438 Raulerson May 1987 A
4682606 DeCaprio Jul 1987 A
4693237 Hoffman et al. Sep 1987 A
4718419 Okada Jan 1988 A
4724836 Okada Feb 1988 A
4813062 Gilpatrick Mar 1989 A
4847049 Yamamoto Jul 1989 A
4853470 Strupczewski Aug 1989 A
4863470 Carter Sep 1989 A
4909250 Smith Mar 1990 A
4926858 Gifford, III et al. May 1990 A
5007908 Rydell Apr 1991 A
5024617 Karpiel Jun 1991 A
5035696 Rydell Jul 1991 A
5041124 Kensey Aug 1991 A
5047027 Rydell Sep 1991 A
5057082 Burchette, Jr. Oct 1991 A
5059204 Lawson et al. Oct 1991 A
5064424 Bitrolf Nov 1991 A
5066295 Kozak et al. Nov 1991 A
5078716 Doll Jan 1992 A
5080660 Buelna Jan 1992 A
5085659 Rydell Feb 1992 A
RE33925 Bales et al. May 1992 E
5133359 Kedem Jul 1992 A
5133360 Spears Jul 1992 A
RE34056 Lindgren et al. Sep 1992 E
5147307 Gluck Sep 1992 A
5158561 Rydell et al. Oct 1992 A
5163938 Kambara et al. Nov 1992 A
5195533 Chin et al. Mar 1993 A
5196007 Ellman et al. Mar 1993 A
5197846 Uno et al. Mar 1993 A
5201732 Parins et al. Apr 1993 A
5201741 Dulebohn Apr 1993 A
5207686 Dolgin May 1993 A
5217458 Parins Jun 1993 A
5224488 Neuffer Jul 1993 A
5236410 Granov et al. Aug 1993 A
5281218 Imran Jan 1994 A
5281408 Unger Jan 1994 A
5282781 Liprie Feb 1994 A
5312400 Bales et al. May 1994 A
5318564 Eggers Jun 1994 A
5320613 Houge et al. Jun 1994 A
5323768 Saito et al. Jun 1994 A
5324288 Billings et al. Jun 1994 A
5334381 Unger Aug 1994 A
5335671 Clement Aug 1994 A
5344420 Hilal et al. Sep 1994 A
5368030 Zinreich et al. Nov 1994 A
5374188 Frank et al. Dec 1994 A
5376094 Kline Dec 1994 A
5380321 Yoon Jan 1995 A
5389106 Tower Feb 1995 A
5395312 Desai Mar 1995 A
5395319 Hirsch et al. Mar 1995 A
5415656 Tihon et al. May 1995 A
5417687 Nardella et al. May 1995 A
5417697 Wilk et al. May 1995 A
5422730 Barlow et al. Jun 1995 A
5423809 Klicek Jun 1995 A
5423814 Zhu et al. Jun 1995 A
5431649 Mulier et al. Jul 1995 A
5433204 Olson Jul 1995 A
5437665 Munro Aug 1995 A
5441498 Perkins Aug 1995 A
5441503 Considine et al. Aug 1995 A
5462553 Dolgin Oct 1995 A
5470308 Edwards et al. Nov 1995 A
5477862 Haaga Dec 1995 A
5484436 Eggers et al. Jan 1996 A
5487385 Avitall Jan 1996 A
5488958 Topel et al. Feb 1996 A
5494030 Swartz et al. Feb 1996 A
5501654 Failla et al. Mar 1996 A
5507743 Edwards et al. Apr 1996 A
5526822 Burbank et al. Jun 1996 A
5527331 Kresch et al. Jun 1996 A
5538010 Darr et al. Jul 1996 A
5542948 Weaver et al. Aug 1996 A
5549560 Van De Wijdeven Aug 1996 A
5578030 Levin Nov 1996 A
5595185 Erlich Jan 1997 A
5597378 Jervis Jan 1997 A
5599347 Hart et al. Feb 1997 A
5607389 Edwards et al. Mar 1997 A
5611803 Heaven et al. Mar 1997 A
5636255 Ellis Jun 1997 A
5643246 Leeb et al. Jul 1997 A
5643282 Kieturakis Jul 1997 A
5646146 Faarup et al. Jul 1997 A
5649547 Ritchart et al. Jul 1997 A
5653718 Yoon Aug 1997 A
5665085 Nardella Sep 1997 A
5674184 Hassler, Jr. Oct 1997 A
5676663 Kim Oct 1997 A
5683384 Gough et al. Nov 1997 A
5687739 McPherson et al. Nov 1997 A
5688490 Tournier et al. Nov 1997 A
5715825 Crowley Feb 1998 A
5720763 Tovey Feb 1998 A
5741225 Lax et al. Apr 1998 A
5749626 Yoshida May 1998 A
5769086 Ritchart et al. Jun 1998 A
5772660 Young et al. Jun 1998 A
5775333 Burbank et al. Jul 1998 A
5782764 Werne Jul 1998 A
5782775 Milliman et al. Jul 1998 A
5794626 Kieturakis Aug 1998 A
5797907 Clement Aug 1998 A
5800378 Edwards et al. Sep 1998 A
5810806 Ritchart et al. Sep 1998 A
5814044 Hooven Sep 1998 A
5846513 Carroll et al. Dec 1998 A
5848978 Cecchi Dec 1998 A
5853366 Dowlatshahi Dec 1998 A
5857981 Bucalo et al. Jan 1999 A
5857982 Milliman et al. Jan 1999 A
5876340 Tu et al. Mar 1999 A
5882316 Chu et al. Mar 1999 A
5902272 Eggers et al. May 1999 A
5913857 Ritchart et al. Jun 1999 A
5921915 Aznoian et al. Jul 1999 A
5925044 Hofmann et al. Jul 1999 A
5928164 Burbank et al. Jul 1999 A
5947964 Eggers et al. Sep 1999 A
5954670 Baker Sep 1999 A
5964716 Gregoire et al. Oct 1999 A
5972002 Bark et al. Oct 1999 A
5980469 Burbank et al. Nov 1999 A
5984919 Hilal et al. Nov 1999 A
5997560 Miller Dec 1999 A
6004269 Crowley et al. Dec 1999 A
6036681 Hooven Mar 2000 A
6050955 Bryan et al. Apr 2000 A
6056700 Burney et al. May 2000 A
6063082 DeVore et al. May 2000 A
6077179 Liechty, II Jun 2000 A
6120462 Hibner et al. Sep 2000 A
6142955 Farascioni et al. Nov 2000 A
6161034 Burbank et al. Dec 2000 A
6220248 Voegele et al. Apr 2001 B1
6234177 Barsch May 2001 B1
6261241 Burbank et al. Jul 2001 B1
6277083 Eggers et al. Aug 2001 B1
6280399 Rossin et al. Aug 2001 B1
6312429 Burbank et al. Nov 2001 B1
6331166 Burbank et al. Dec 2001 B1
6344026 Burbank et al. Feb 2002 B1
6350244 Fisher Feb 2002 B1
6387056 Kieturakis May 2002 B1
6419490 Kitchings Weathers, Jr. Jul 2002 B1
6454727 Burbank et al. Sep 2002 B1
6478806 McFarlane Nov 2002 B2
6494881 Bales et al. Dec 2002 B1
6514215 Ouchi Feb 2003 B1
6514248 Eggers et al. Feb 2003 B1
6517545 Mazur Feb 2003 B1
6540695 Burbank et al. Apr 2003 B1
6638234 Burbank et al. Oct 2003 B2
6659981 Stewart et al. Dec 2003 B2
6679851 Burbank et al. Jan 2004 B2
6689145 Lee et al. Feb 2004 B2
6712775 Burbank et al. Mar 2004 B2
6758824 Miller et al. Jul 2004 B1
7070010 Papousek Jul 2006 B2
7189206 Quick et al. Mar 2007 B2
7201722 Krueger Apr 2007 B2
7226424 Ritchart et al. Jun 2007 B2
8343071 Shabaz et al. Jan 2013 B2
20010002250 Burbank et al. May 2001 A1
20030004407 Carroll et al. Jan 2003 A1
20040019299 Ritchart et al. Jan 2004 A1
20090204021 Shabaz et al. Aug 2009 A1
Foreign Referenced Citations (42)
Number Date Country
1225813 Sep 1966 DE
19528440 Feb 1997 DE
0146699 Jul 1985 EP
0255123 Feb 1988 EP
0292936 Nov 1988 EP
0472368 Feb 1992 EP
0509670 Oct 1992 EP
0601709 Jun 1994 EP
0667126 Aug 1995 EP
0769281 Apr 1997 EP
0858774 Aug 1998 EP
0919190 Jun 1999 EP
0919192 Jun 1999 EP
0966925 Dec 1999 EP
0970658 Jan 2000 EP
0983749 Mar 2000 EP
2311468 Oct 1997 GB
H11262490 Sep 1999 JP
2001158016 Jun 2001 JP
2005530554 Oct 2005 JP
9314712 Aug 1993 WO
9502370 Jan 1995 WO
9502371 Jan 1995 WO
9503842 Feb 1995 WO
9503843 Feb 1995 WO
9729702 Aug 1997 WO
9806346 Feb 1998 WO
9808441 Mar 1998 WO
9843531 Oct 1998 WO
9930764 Jun 1999 WO
9944506 Sep 1999 WO
0012009 Mar 2000 WO
0016697 Mar 2000 WO
0149184 Jul 2001 WO
0222023 Mar 2002 WO
02062231 Aug 2002 WO
02062232 Aug 2002 WO
02092957 Nov 2002 WO
2004052212 Jun 2004 WO
2004075719 Sep 2004 WO
2005063126 Jul 2005 WO
2006049911 May 2006 WO
Non-Patent Literature Citations (36)
Entry
Written Opinion of the International Searching Authority for PCT/US99/21416 dated Jul. 18, 2000.
International Search Report for PCT/US2004/043021 dated Apr. 27, 2005.
International Search Report for PCT/US2004/043021 dated Jul. 26, 2005.
Written Opinion of the International Searching Authority for PCT/US2004/043021 dated Jul. 26, 2005.
International Search Report for PCT/US2005/027071 dated Mar. 21, 2006.
International Search Report for PCT/US2005/027071 dated Jul. 5, 2006.
Written Opinion of the International Searching Authority for PCT/US2005/027071 dated Feb. 3, 2007.
Storm, et al., “Clinical Thermochemotherapy, A Controlled Trial in Advanced Cancer Patients”, Cancer, Feb. 15, 1984, pp. 863-868, vol. 53.
Doss, et al., “HDR Brachytherapy for Osteolytic Metastases in Previously Irradiated Sites”, International Brachytherapy, Chapter 101, Sep. 1992, pp. 412-415, Memorial Regional Cancer Center, Modesto, CA.
Kuske, et al. “Brachytherapy as Sole Method for Early Breast Cancer”, International Brachytherapy, Chapter 80, pp. 347-348, Ochsner Medical Institutions, New Orleans, Louisiana.
Desinger, et al., “A New Application System for Simultaneous Laser and Ultrasonic Transmission in Endoscopic Surgery (LUST)”, Surgical Applications of Energy, 94, vol. 3249 Apr. 2, 1998, San Jose, CA.
Desinger, et al., “Interstitial bipolar RF-thermotherapy (RFITT) Therapy planning by computer simulation and MRI-monitoring—A new concept for minimally invasive procedures—” 2 Surgical Applications of Energy, 147, vol. 3249, Apr. 2, 1998, San Jose, CA.
“The Dangers of Monopolar Electrosurgery and the Advantages of Bipolar Electrosurgery”, Everest Medical, Technical Reviews; www.pycco.com/emc/techrvws.html, May 26, 1998, pp. 1-9.
Hausner, K, “Laser Vs Electrosurgery”, www.netvs.com/elmed/lasvselec.htm, May 19, 1998, pp. 1-4.
Bown, S. G. , “Phototherapy of Tumors”, World Journal of Surgery, 1983, vol. 7, pp. 700-709, University College Hospital, London, United Kingdom.
Jacques, et al., “Liver photocoagulation with diode laser (805 nm) vs Nd:YAG laser (1064 nm)”, SPIE vol. 1646 Laser-Tissue Interaction III 1992, pp. 107-125.
Jolesz, et al., “MR Imaging of Laser-Tissue Interactions”, Magnetic Resonance Imaging, Radiology, Jul. 1988; pp. 249-253, vol. 168.
Anzai, et al., “Nd:YAG Interstitial Laser Phototherapy Guided by Magnetic Resonance Imaging in an Ex Vivo Model: Dosimetry of Laser-MR-Tissue Interaction”, Laryngoscope 101: Jul. 1991, pp. 755-760.
Le Bihan, et al., “Temperature Mapping with MR Imaging of Molecular Diffusion; Application to Hyperthermia”, Therapeutic Radiology, Radiology, Jun. 1988, pp. 853-857, vol. 171.
Masters, et al., “Interstitial Laser Hyperthermia in Tumour Therapy”, Annales Chirugiae et Gynaecologiae 79: 244-251, 1990.
Harries, et al., “Interstitial laser photocoagulation as a treatment for breast cancer”, British Journal of Surgery 1994, 81, 1617-1619.
“Ultrasound-Guided Cryosurgery for Tumor Ablation”, Mar. 22, 1995, Sheraton Boston Hotel & Towers, Boston, MA, Sponsored by: Deconess Hospital.
Gehman, et al., “High Dose Rate Endovascular Irradiation; Tolerance of Normal Tissues”, Endocurietherapy/ Hyperthermia Oncology, Jul. 1994, vol. 10, pp. 167-171, ISSN 8756-1687.
Bottcher, et al. “Endovascular Irradiation—A New Method to Avoid Recurrent Stenosis After Stent Implantation in Peripheral Arteries: Technique and Preliminary Results”, 34th Annual ASTRO Meeting, San Diego, CA, Nov. 1992, International Journal of Radiation Oncology Biol. Phys., vol. 29, No. 1, pp. 183-186, 1994.
Fletcher, G. H., “Textbook of Radiotherapy” Third Edition, Lea & Febiger, 1980, Philadelphia.
Cox, J. D., “Moss' Radiation Oncology: Rationale, Technique, Results” Seventh Edition, Mosby 1994.
Amin, Zehir, MRCP et al., “Hepatic Metastases: Interstitial Laser Photocoagulation with Real-Time US Monitoring and Dynamic CT Evaluation of Treatment”, Radiology, May 1993; vol. 187, pp. 339-347.
Armstrong, J.S. et al., “Differential marking of excision planes in screened breast lesions by organically coloured gelantins”, Journal of Clinical Pathology, (Jul. 1990), 43(7) 604-7, XP000971447 abstract; tables 1 and 2.
Burbank, F., M.D., Stereotactic Breast Biopsy: Its History, Its Present, and Its Future, The American Surgeon, Feb. 1996, vol. 62, pp. 128-150.
Fucci, V. et al., “Large Bowel Transit Times Using Radiopaque Markers in Normal Cats”, J. of Am. Animal Hospital Assn., Nov.-Dec. 1995 vol. 31 (6) 473-477.
Lorenzen,T. et al., The Loop Electrode: a New Device for US-guided Interstitial Tissue Ablation Using Radio frequency Electrosurgery—An Animal Study, 1996 Blackwell Science Ltd. Min Invas Ther & Allied Technol, pp. 5.511-5.516.
Micklos, Timothy J., Percutaneous Biopsy Techniques, Manual of Oncologic Therapeutics (1989/1990) pp. 39-42.
Nolsoe, Christian P., et al., “Interstitial Hyperthermia of Colorectal Liver Metastases with a US-guided Nd-YAG Laser with a Diffuser Tip: A Pilot Clinical Study”, Radiology, May 1993, vol. 187, pp. 333-337.
Schindlebeck, N. E., et al., “Measurement of Colon Transit Time”, J. of Gastroenterology, No. 28, pp. 399-404, 1990.
Canavan, et al., Dr. F., “Vaccuum Assisted Breast Biopsy: A Comparison of 3 Systems”, Presentation poster, Kings College Hospital NHS Foundation Trust; Aug. 2008.
Whitman, et al., Coaxial Core Needle Biopsy Under Mammographic Guidance: Indications and Applications, AJR:171, Jul. 1998, pp. 67-70.
Related Publications (1)
Number Date Country
20130138014 A1 May 2013 US
Divisions (1)
Number Date Country
Parent 11014413 Dec 2004 US
Child 11981024 US
Continuations (1)
Number Date Country
Parent 11981024 Oct 2007 US
Child 13747530 US