Vacuum assisted biopsy device

Description

TECHNICAL FIELD

The present disclosure generally relates to the field of tissue sampling and harvesting. More specifically, the disclosure relates to biopsy needle sets and devices.

BACKGROUND

In the practice of diagnostic medicine, it is often necessary or desirable to perform a biopsy, or to sample selected tissue from a patient for medical evaluation. Cytological and histological studies of the biopsy sample can then be performed as an aid to the diagnosis and treatment of disease. Biopsies can be useful in diagnosing and treating various forms of cancer, as well as other diseases in which a localized area of affected tissue can be identified.

Biopsies are routinely performed on tissue using a needle set, which typically includes a stylet with a pointed tip and a notch defined near its distal end. The stylet is slidably disposed within a cannula so that the notch can be alternately exposed or covered. Such needle sets are used with or incorporated in various forms of biopsy devices, such as single action or double action biopsy devices.

More specifically, one known exemplary single action biopsy device includes a hollow needle. A stylet is slidingly disposed within the hollow needle lumen and is moveable relative to needle. A distal end of the stylet is provided with a tissue cutting-point and a tissue opening is positioned adjacent to the distal end for receiving tissue samples. The stylet is slidable relative to needle between a first or retracted position and a second or extended position.

In the first position, the stylet is retracted within the needle such that the needle covers the tissue opening. In the second position, the distal end of the stylet is extended away from the needle to expose the tissue opening to tissues at the biopsy site.

During a biopsy procedure, the device will be positioned within a cavity at a targeted site for the biopsy. The stylet is momentarily driven into the tissue and tissue then prolapses into the tissue opening. The needle is then advanced along the stylet to cover the tissue opening. This forward movement of needle severs the prolapsed tissue to obtain a tissue sample, which becomes trapped in tissue opening of the stylet. With the needle 22 blocking the opening of tissue opening, the biopsy device is then withdrawn from the target site, carrying the sample within tissue opening. To collect the biopsy sample, the needle is once again retracted to expose tissue opening of the stylet. The procedure may be repeated several times until satisfactory samples have been obtained.

While single and double action biopsy devices are widely used, a basic problem remains in the field of biopsy, which is the need to obtain a sufficient amount of sample tissue. One potential cause of the problem is that as the needle passes over the tissue opening, the needle has a tendency to push the tissue away from the tissue opening. This results in samples that are inferior in quality or too small, which precludes the pathologist from conclusively determining whether disease is present, and if so, to what extent it has progressed. The pathologist must then issue an inconclusive diagnostic report. This causes the physician to recall the patient and attempt another needle biopsy, or in some situations, the patient is scheduled for a more invasive, traumatic and expensive procedure such as an open surgical biopsy.

The challenge has been to consistently obtain sufficient tissue volume and quality tissue cores, regardless of tissue type, to meet the needs of the pathologist so that a conclusive diagnosis can be achieved.

SUMMARY

A biopsy device is disclosed that comprises a cutting element mounted to a handpiece and a vacuum chamber. The cutting element comprises a stylet assembly and an outer cannula assembly. The stylet assembly includes a stylet that includes an open proximal end and a tissue opening at a distal end thereof. The tissue receiving opening is in communication with a lumen extending through the stylet. The outer cannula assembly includes an outer cannula that is slidably mounted over the stylet and has an open distal end with a cutting edge formed thereon. The vacuum chamber is in communication with the lumen of the stylet. The stylet is selectively advanced distally outwardly with respect to outer cannula to expose the tissue opening to targeted tissue. The outer cannula is selectively advanced over the tissue opening to sever tissue, while vacuum is generated in the vacuum chamber and delivered to the tissue opening through the lumen. The vacuum causes tissue to be drawn into and maintained in the tissue opening while the outer cannula severs tissue to obtain a biopsy core. A method of using the biopsy device is also disclosed.

BRIEF DESCRIPTION OF THE DRAWINGS

Embodiments of the disclosure will now be described, by way of example, with reference to the accompanying drawings, wherein:

FIG. 1 is a perspective view of a biopsy device assembly, including a biopsy device and an introducer assembly.

FIG. 2 is an exploded view of the biopsy device of FIG. 1.

FIG. 3 is a perspective view of the underside of a pickup carriage assembly for use with the biopsy device.

FIG. 4 is an exploded view of the pickup carriage assembly, illustrating a moveable cam member and a spring member that attaches to a top surface of the pickup carriage.

FIG. 5 is a perspective view of the underside of the pickup carriage.

FIG. 6 is a perspective view of the moveable cam member.

FIG. 7 is a perspective view of a stylet and vacuum hub assembly.

FIG. 8 is a perspective view of the stylet and vacuum hub assembly of FIG. 7 with a vacuum chamber enclosure member attached and a cutting cannula assembly attached.

FIG. 9 is a perspective view of the cutting cannula assembly of FIG. 8.

FIG. 10 is a perspective view of one embodiment of a resilient bridge member.

FIG. 11 is a partial cut-away perspective view of the biopsy device with the introducer assembly attached to the front portion thereof.

FIG. 12 is a partial cut-away side elevational view of the biopsy device after a release latch has been activated and an actuating lever has been released (note that the bridge member of FIG. 10 has been omitted for clarity).

FIG. 13 is a side elevational view of the biopsy device after the actuating lever has been depressed a first time, thereby retracting a piston.

FIG. 14 is a side elevational view of the biopsy device after the actuating lever has been depressed a second time, thereby retracting the cutting cannula.

FIG. 15 is a side elevational view of the biopsy device after the actuating lever has been depressed a third time, thereby retracting the stylet into the cutting cannula.

FIG. 16 is a side elevational view of the biopsy device after the stylet has been fired away from a housing of the biopsy device.

FIG. 17 is a side elevational view of the biopsy device after the cutting cannula has been fired forward over the tissue receiving opening of the stylet.

FIG. 18 is a side elevational view of the biopsy device after the release latch has been released (note that the bridge member of FIG. 10 has been omitted for clarity).

FIG. 19 is a side elevational view of the biopsy device after the vacuum chamber has been retracted.

FIG. 20 is a side elevational view of the biopsy device after the cutting cannula has been retracted so as to expose the tissue receiving opening to permit tissue cores to be removed from the tissue receiving opening.

FIG. 21A-21D are various views of a valve member.

FIG. 22 is a partial cut-away side elevational view of an alternative embodiment of a biopsy device, after the actuating lever has been depressed a second time, thereby retracting the cutting cannula;

FIG. 23 is a side elevational view of the biopsy device in FIG. 22, after the actuating lever has been depressed a third time, thereby retracting the distal end inner cannula, within the cutting cannula.

DETAILED DESCRIPTION

Referring now to the drawings, preferred illustrative embodiments are shown in detail. Although the drawings represent some embodiments, the drawings are not necessarily to scale and certain features may be exaggerated, removed, or partially sectioned to better illustrate and explain the present disclosure. Further, the embodiments set forth herein are not intended to be exhaustive or otherwise limit or restrict the claims to the precise forms and configurations shown in the drawings and disclosed in the following detailed description.

Referring to FIG. 1, a perspective view of an exemplary biopsy device 10 in accordance with the present disclosure is illustrated. A separate and optional introducer assembly 12 is also illustrated.

As shown, biopsy device 10 is a handheld device and includes a housing 14 to which a stylet 16 is attached. Biopsy device 10 includes several release members 18, 20, and 22, to be explained in further detail below.

Referring to FIG. 2, an exploded view of biopsy device 10 is illustrated. As shown, in the exemplary embodiment housing 14 is a two piece member, including a first housing member 14a and a second housing member 14b. In one embodiment, first and second housing members 14a and 14b are configured snap together to house actuation components of biopsy device 10. For example, first housing member 14a includes one or more slot members 24 positioned on top and bottom portions of first housing member 14a. Slot members 24 cooperate with and receive latch members 26 that are positioned on top and bottom portions of second housing member 14b. An interior of housing 14 is generally hollow to receive the actuation components.

While housing 14 has been described as snapping together, it is also understood that first and second housing members 14 may alternatively be secured together using fastening elements.

A top portion of each housing member 14a and 14b includes a holder 28 for securing a portion of a resilient bridge member 30. Each holder 28 extends upwardly from the top portion 32 and includes a groove 34 (best seen in FIG. 12) that receives mounting knobs 36 of a mounting member 38 positioned on a first end 35 of resilient bridge member 30.

An actuating lever 40 is pivotally attached to housing 14 by pivot arm 42 at a proximal end 44 of biopsy device 10. A forward end 46 of actuating lever 40 may rise upwardly from a top surface of housing 14 due to pivot arm 42. A lever release assembly 48 that carries a release mechanism 18 is attached to actuating lever 40. Lever release assembly 48 includes a downwardly extending latch arm 46 that selectively engages with a portion of a retaining member 50 disposed on a cam member 52 carried by a pickup carriage 54 (shown in FIGS. 3-5). A spring mechanism 53 serves to bias release mechanism 18 to an actuation position.

Pickup carriage 54 includes a pair of holders 56 that extend upwardly from a top surface thereof. Housing 14 includes an open channel 58 formed in the top surface thereof. When pickup carriage 54 is positioned within housing 14, holders 56 extend through channel 58 (seen in FIG. 12). Each holder 56 includes a groove 60 that receives a mounting knob 36 from a mounting member 38 positioned on a second end 62 of resilient bridge member 30.

Referring to FIG. 10, resilient bridge member 30 includes a plurality of sections that are separated by hinge members 64a and 64b. Hinge members 64a and 64b are created by V-shaped notches that form thinned sections.

First end 35 of resilient bridge member 30 is secured to holders 28 and second end 62 is secured to holders 56 such that resilient bridge member 30 is positioned directly below actuation lever 40 when biopsy device 10 is assembled. Due to the configuration of resilient bridge member 30, when actuation lever 40 is depressed, actuation lever 40 pushes down on resilient bridge member 30. The pushing action flattens out resilient bridge member 30, thereby sliding pickup carriage member 54 away from a distal end of biopsy device 10.

Secured to a top portion of housing 14 is an actuation button carrier 66 that carries release mechanisms 20 and 22. Release mechanism 20 includes a downwardly extending latch arm 68 that extends downwardly into first housing member 14a though an opening 70 formed therein. As will be explained in further detail below, release mechanism 20 is actuated to release stylet 16. More specifically, an end of latch arm 68 is configured to grip a retaining arm 72 of stylet 16. When release mechanism 20 is depressed, the end of latch arm 68 is biased upwardly, thereby releasing its grip on retaining arm 72 of stylet 16 and permitting stylet to advance forward.

Release mechanism 22 also includes a downwardly extending latch arm (not shown). As will be explained n further detail below, the latch arm of release mechanism 22 releases an outer cutting cannula 74. More specifically, when release mechanism 22 is depressed, the end of the latch arm of release mechanism 22 is biased upwardly, thereby releasing outer cutting cannula 74 and permitting outer cannula 74 to advance forward.

Other components of biopsy device 10 includes a stylet assembly 76, an outer cannula assembly 78, a cam member assembly 80, a support rib 82, and a piston member 84. Each element will be discussed in turn below.

Stylet assembly 76 is shown in FIG. 7. Stylet assembly 76 includes stylet 16, a first arm sub-assembly 86, and a second arm sub-assembly 88. Stylet 16 extends between a distal end 90 and an open proximal end 92. Adjacent distal end 90 is a tissue opening 94. Distal end 90 may further include a trocar piercing tip 95. Stylet 76 further defines an inner lumen 96 that extends between tissue opening 94 and proximal end 92. Positioned adjacent proximal end 92 are first and second seal members 98, 100, respectively. First seal member 98 is attached a first cap member 102 that is attached to second arm sub-assembly 88. Second seal member 100 positioned adjacent to a chamber wall member 103, which is positioned adjacent second end cap 104. Second end cap 104 is fixedly secured to stylet 16. Second seal member 100 (see FIG. 2) is disposed between first end cap 102 and chamber wall member 103. Thus, first end cap 102, chamber wall member 103, and first and second seal members 98, 100 cooperate with a cylinder 106 to define a vacuum chamber 108, to be explained in further detail below.

A notch 110 is cut into stylet 16, between first end cap 102 and chamber wall member 103. Notch 110 is in communication with inner lumen 96, which, in turn, is in communication with tissue opening 94. A one-way valve member 109 (to be discussed in further detail below) is attached to open proximal end 92 (see, e.g., FIG. 2).

First arm sub-assembly 86 includes is generally L-shaped and includes a leg member 112 and a carrier member 114. Carrier member 114 is fixedly secured to stylet 16. Carrier member 114 includes a fitting member 116 that cooperative engages a side of complimentary member 118 that is disposed on a carrier member 120 that is part of second arm sub-assembly 88.

Second arm sub-assembly 88 includes a long leg member 122 and a short leg member 124 that are connected together by carrier member 120. When assembled (and as best seen in FIG. 7), short leg member 124 is disposed beneath leg member 112 of first arm sub-assembly 86, with carrier member 114 being positioned above carrier member 120. First cap member 102 is attached to carrier member 120. First cap member 120 is fixedly secured to cylinder 106. Thus, as vacuum chamber 108 moves, so does second arm sub-assembly 88.

Referring to FIG. 9, outer cannula assembly 74 includes an outer cutting cannula 126 that is fixedly attached to an outer cannula hub 128 at its proximal end. Outer cannula hub 128 includes a positioning member 130 on one side and a retaining member 132 on another. Retaining member 132 includes a retaining finger 134. A distal end 136 of outer cannula 126 is sharpened to sever tissue.

Referring to FIG. 2, outer cannula assembly 74 is assembled to stylet assembly 76 as follows. First, a bumper member 138 is positioned over stylet 16 and into contact with a mounting face 140. Support rib 82 is next slid onto stylet 16. Support rib 82 (best seen in FIG. 2) includes first and second mounting grooves 142, 144. First mounting groove 142 is configured to receive short leg member 124 of second arm sub-assembly 86 and leg member 112 of first arm sub-assembly 86. Second mounting groove 144 is configured to receive long leg member 122 of second arm sub-assembly 86. An outwardly extending spring mount 146 is formed on support rib 82. A biasing member 148, such as a spring is positioned on spring mount 146. Outer cannula hub 128 includes a spring mount 150 that receives and end of biasing member 148.

Referring now to FIGS. 3-6, pickup carriage 54 and cam member 52 will be described. Pickup carriage 54 includes a first elongated groove 152 and a second shortened groove 154. A mounting hole 156 is positioned opposite second groove 154. An access opening 158.

Cam member 52 includes a mounting member 160 that is received within mounting hole 156. A first pivot member 162 from cam member 52 is positioned within first groove 152 of pickup carriage 54. A second pivot member 164 from cam member 52 (seen in FIG. 2) is positioned within second groove 154. Retaining member 50 is positioned on an end of cam member 52 and is received within access opening 158.

A biasing member 166 received on a mounting portion 168 of pickup carriage 54. A distal end 170 of biasing member 166 contacts first pivot member 162 and biases first pivot member 162 toward a first end 172 of first groove 152. Pickup carriage 54 may further include a tang member 174 that partially retains a portion of biasing member 166.

A proximal end 176 of pickup carriage 54 includes a mounting post 178. A biasing member 180 is received on mounting post 178. An end of biasing member 180 engages an internal wall 182 formed by first and second housing members 14a and 14b when pickup carriage 54 is installed therewithin. When pickup carriage 54 is installed, holders 56 are oriented to extend upwardly through channel 58 formed through housing 14. Cam member 52 is installed on a bottom surface 184 of pickup carriage 54 as shown in FIG. 3.

Referring to FIGS. 12-20, operation of biopsy device 10 will now be described. Assuming biopsy device 10 is packaged in the fired position (see FIG. 12), biopsy device 10 must first be moved into the cocked position. To move biopsy device 10 into the cocked position, first release latch 18 is actuated to release actuation lever 40 from housing 14 (see FIG. 12). Actuation lever 40 is then depressed, pushing down on bridge member 30, which is attached to holders 56 of pickup carriage 54. Accordingly, when bridge member 30 is depressed, pickup carriage 54 is moved toward proximal end 44 of biopsy device 10.

As pickup carriage 54 moves toward proximal end 44 of biopsy device 10, a first pickup member 186 contacts a first tang member 188 that is carried on carrier member 120 that is part of second arm sub-assembly 88, and retracts vacuum chamber 108 proximally, as shown in FIG. 13. A first piston spring member 190 that is at least partially positioned over vacuum chamber 108, is compressed between a proximal face 192 of carrier member 120 and a first lower internal face 194 positioned within housing 14. A second spring member 196 is compressed between second end cap 104 and a second lower internal face 198 positioned within housing 14. This action also collapses the vacuum chamber 108, moving first end cap 102 towards chamber wall member 103. Air within vacuum chamber 108 is directed out through seal member 109 that is secured to proximal end 92 of stylet 16.

In one embodiment, seal member 109 is a configured as a duck-bill style valve member 109 (FIG. 2). Valve member 109 includes a body member 103 having an open distal end 105 that is connected to a tapered, duck bill, normally closed proximal end 107. Proximal end 107 includes a slit which is forced open when positive pressure is generated within stylet 16. Open distal end 105 is secured to proximal end 92 of stylet 16.

An alternative embodiment of seal member 109′ is shown in FIGS. 21A-21D. Seal member 109′ includes a body member 111 having an open distal end 119 and a normally closed proximal end. Adjacent to the proximal end of seal member 109′ is a slit 113 that cooperates with a land member 115 to form a flap member 117. Slit 113 extends along a substantial portion of body member 111 such that land member 115 acts as a hinge for flap member 117. In operation, as positive pressure is generated within the system, flap member 117 will be forced open.

Spring member 180 biases pickup carriage 54 back toward a distal end of biopsy device 10. Actuation lever 40 is depressed again. The second depression of actuation lever 40 causes pickup carriage 54 to move in the proximal direction again. As pickup carriage 54 moves, a second pickup member 200 positioned on cam member 54 contacts a second tang member 202 that is carried on outer cannula hub 128. Such action retracts outer cannula assembly 74, moving distal end 136 thereof away from distal end 90 of stylet 16. Retaining member 132 is compressed inwardly until retaining finger 134 grips an internal ledge (not shown) formed in first housing member 14a. Retraction of outer cannula assembly 74 causes biasing member 148 to compress between a proximal face 204 of outer cannula hub 128 and a distal face 206 of support rib 82.

Spring member 180 biases pickup carriage 54 once again and actuation lever 40 is depressed a third time. The third depression of actuation lever 40 causes pickup carriage 54 to move proximally once again. As pick up carriage 54 moves proximally, first pickup member 186 engages with fitting member 116 that is carried on carrier member 114 of first arm sub-assembly 86 and pulls first arm sub-assembly 86 towards second arm sub-assembly 88. Once carrier 114 of first arm sub-assembly 86 reaches carrier 120 of second arm sub-assembly 88, stylet 16 is pulled into outer cannula 126 and stylet 16 is locked into the cocked position. On the third depression, actuation lever 40 locks down and latch release assembly 48 retains lever 40 against housing 14 (see FIG. 15), thereby providing a tactile indicator that biopsy device is in the cocked position.

Biopsy device may also include a visual indicator to indicate that biopsy device 10 is in the cocked position. In one embodiment, at least leg member 112 of first arm sub-assembly 86 may be constructed of a particular color that is different than the color of housing 14 and that will be visible through a window 208 only when biopsy device 10 is in the cocked position. For example, leg member 112 may be formed from a green material such that a portion of the green material is visible through window 208 when biopsy device 10 is in the cocked position so as to be in the “biopsy ready position.” In contrast, when stylet 16 is in a non biopsy ready position, leg member 112 will be positioned away from indicator window 208.

Once in the cocked position, or biopsy ready position, a biopsy may be performed. The operation will now be explained.

Typically, before a biopsy is performed, a targeted area must be identified. Any suitable method may be used to identify a targeted area for biopsy. Such methods include, but are not limited to, the methods and use of the devices described in co-pending application Ser. No. 10/649,068, the contents of which are incorporated herein by reference in its entirety.

Next, the entry site is prepared, as required (such as applying anesthesia, cleaning the biopsy area, etc.). During this step, an introducer assembly 12 (see FIG. 1) may be positioned over outer cannula 112 to provide a pathway to the target area. Introducer assembly 12 will be explained in further detail below.

Next, a tip of stylet 16 is placed at the targeted area. In one embodiment, stylet 16 may be fired prior to inserting biopsy device 10 into the patient. In another embodiment, stylet 16 is not fired until after biopsy device 10 is inserted into the patient. In one embodiment, the position and orientation of biopsy device 10 is maintained during the firing process.

A stylet release or firing member 20 is depressed, thereby releasing stylet assembly 76 from its cocked position into the fired position (FIG. 16). Such action exposes tissue opening 94 into which tissue may prolapse. Tissue receiving opening 94 is connected to inner lumen 96. Inner lumen 96 is connected to vacuum chamber 108.

To differentiate between stylet release member 20 and an outer cannula release member 22, stylet release member 20 may be a different color than housing 14 or outer cannula release member 22 (to be described below) to allow a user to visually differentiate between the two release members. In one embodiment, one of stylet and outer cannula release members 20, 22 may alternatively include a tactile indicator, such as a raised bump 210 on the release member, to allow a user to feel the differences between the two release members (see, e.g., FIGS. 1 and 11).

After stylet release member 20 is actuated, outer cannula release member 22 is then actuated. This action will release outer cannula assembly 78. Outer cannula assembly 78 is forced over stylet 16 by biasing members/springs 148, 190, and 196, such that outer cannula assembly 78 rapidly fires forward. As outer cannula assembly 78 is fired forward, vacuum chamber 108 is expanded so as to create a vacuum by drawing air through tissue opening 94 and lumen 96, and entering into vacuum chamber 108 through notch 110. A further explanation of the vacuum chamber may be found in commonly owned and co-pending U.S. application Ser. No. 11/389,274, the contents of which are incorporated herein by reference in its entirety.

In one embodiment (not shown), a vacuum valve having a slit that creates a flap may be provided that selectively covers the notch. When stylet 16 is fired forward, positive pressure generated inside vacuum chamber 108 closes the valve flap to prevent pressure from reaching the inside of lumen 96. When outer cannula 74 fires forward, the negative pressure inside vacuum chamber 108 opens the valve, allowing vacuum to be delivered to tissue opening 94 in stylet 16, through lumen 96.

As outer cannula assembly 78 is fired and vacuum is generated by the expansion of vacuum chamber 108, the vacuum biases tissue toward tissue opening 94 and holds tissue in place while outer cannula 74 slides over tissue opening 94. As outer cannula 74 slides, sharpened distal end 136 slices through the tissue, thereby severing the tissue so as to leave a biopsy core 212 within tissue opening 94.

Once biopsy core 212 is acquired, to retrieve biopsy core 212 from biopsy device 10, biopsy device 10 is removed from the patient. If an introducer assembly 12 is used, it is kept in position within the patient. Once removed from the patient, release member 18 is depressed once again to release latch member 26. Latch member 26 is depressed twice to pull back outer cannula 74 so as to expose tissue opening 94 (see FIGS. 18-20) and biopsy core 212. To obtain additional biopsy cores 212, the latch member 26 is depressed a third time (FIG. 20) to retract stylet 16 into the biopsy ready position.

Referring to FIGS. 1 and 11, introducer assembly 12 will now be explained. Introducer assembly 12 includes an introducer cannula 214 that is fixedly connected to an introducer hub 216. Introducer cannula 214 is hollow and is sized to slide over outer cannula 74 so as to be spaced proximally from distal end of outer cannula 74. Introducer hub 216 may include a normally closed valve (not shown) and includes an opening that is in communication with introducer cannula 214. Disposed on introducer hub 216 is a selectively releasable latch member 218 that includes a connecting member 220 and a releasing member 222. Releasing member 222 is received within an opening 224 to secure introducer assembly 12 to biopsy device 10.

In operation, introducer assembly 12 is positioned over outer cannula 74 and slid along outer cannula 74 until connecting member 220 of latch member 218 is received within opening 224, thereby connecting introducer assembly 12 to biopsy device 10. Introducer assembly 12 may be connected to biopsy device 10 either before or after biopsy device is placed in the biopsy ready position. Once connected, biopsy device 10 is inserted into the patient with introducer cannula 214. Introducer cannula 214 operates to maintain a pathway to the biopsy site.

Once biopsy cores 212 are taken, biopsy device 10 may be detached from introducer assembly 12 by depressing releasing member 222 such that connecting member 220 is released from opening 224. Once freed, introducer cannula 214 remains within the patient's body, to maintain the pathway to the biopsy site. Use of introducer assembly 12 minimizes trauma to the patient and eliminates the need for multiple reinsertions of biopsy device 10, as well as permits access to the biopsy site for treatment and other post biopsy activities. As such, after the biopsy cores 212 are removed from tissue opening 94, biopsy device 10 may be reinserted into introducer cannula 214 to take addition biopsy cores 212.

Alternatively, if desired, a biopsy marker (not shown) may be deployed into the biopsy cavity after biopsy cores 212 have been taken. In such a case, a site marker deployment device may be inserted within introducer assembly 12 after biopsy device 10 is removed therefrom. Once such example of a site marker deployment device is disclosed in commonly owned and co-pending application Ser. No. 11/238,295, the contents of which are incorporated herein by reference in its entirety.

Referring now to FIGS. 22 and 23, another embodiment of a biopsy device 300 is illustrated. Biopsy device 300 includes the same components as biopsy device 10, except that distal end 301 of stylet 316 is formed with a blunt tip 302 rather than a trocar tip, as shown with stylet 16.

Blunt tip 302 is useful for those instances where a lesion to be biopsied is close to the chest wall. More specifically, the length of blunt tip 302 is shorter than the length required for a trocar tip, thereby permitting access to a lesion close to a chest wall.

However, because there is no trocar tip, to position biopsy device 300 at a target area within the body, a separate trocar device (not shown) must be used to create a pathway for the stylet 316 and cutting cannula 74. An example of a trocar device is shown and described in commonly owned U.S. Pat. No. 7,347,829, the contents of which are incorporated in its entirety. As may be seen, the trocar device is defined by an elongated body having a sharp distal end. The proximal end of the trocar device may also include handle.

In operation, once the target area is defined, the trocar device is inserted into the patient to create a pathway to the target site. In one arrangement, introducer assembly 12 is used with the trocar device. More specifically, and as described in U.S. Pat. No. 7,347,829, trocar device is inserted into the introducer cannula 214 prior to insertion of the trocar device into the patient's body. A target confirmation device (as described and disclosed in U.S. Pat. No. 7,347,829) may then be used to verify that the pathway created by the trocar device has reached the target site. In one embodiment, the trocar device may be used as the target confirmation device. In another embodiment, the target confirmation device is a separate component that may inserted into the pathway after removal of the trocar device. When the trocar device is removed from the patient's body, the introducer cannula 214 will remain within the patient's body to hold open the pathway to the target area.

Once the pathway to the target site is defined, the distal end 301 of the biopsy device 300 is inserted into the introducer cannula 214 until distal end 301 extends outwardly from a distal end of the introducer cannula 214. Releasing member 222 may be inserted into the opening 224 formed on the housing of biopsy device 300 in a similar fashion as described in connection with the biopsy device 10. Once inserted through the introducer cannula 214, the biopsy device 300 may be operated in the same manner as described in connection with biopsy device 300.

While the embodiments of the present invention has been particularly shown and described with reference to the foregoing preferred embodiments, it should be understood by those skilled in the art that various alternatives to the embodiments of the invention described herein may be employed in practicing the invention without departing from the spirit and scope of the invention as defined in the following claims. It is intended that the following claims define the scope of the invention embodiments within the scope of these claims and their equivalents be covered thereby. This description of the invention should be understood to include all novel and non-obvious combinations of elements described herein, and claims may be presented in this or a later application to any novel and non-obvious combination of these elements. The foregoing embodiment is illustrative, and no single feature or element is essential to all possible combinations that may be claimed in this or a later application.

Claims

1. A biopsy device, comprising: a cutting element mounted to a handpiece, said cutting element comprising:a stylet assembly having a stylet that includes an open proximal end and a tissue opening at a distal end thereof, wherein the tissue receiving opening is in communication with a lumen extending through the stylet, wherein the stylet is formed with a blunt distal end; andan outer cannula assembly including an outer cannula that is slidably mounted over the stylet and having an open distal end with a cutting edge formed thereon; anda vacuum chamber in communication with the lumen;wherein the stylet is selectively advanced distally outwardly with respect to the outer cannula to open the tissue opening to targeted tissue;wherein the outer cannula assembly is actuated so as to at least partially expand the vacuum chamber to generate vacuum, wherein the outer cannula is automatically advanced over the tissue opening after the vacuum chamber is at least partially expanded so as to sever tissue, the vacuum causing tissue to be drawn into and maintained in the tissue opening while the cutting cannula severs tissue to obtain a biopsy core.
2. The biopsy device of claim 1, further comprising a pickup carriage that operates to selectively move the stylet assembly and the outer cannula assembly between a biopsy ready and a fired position.
3. The biopsy device of claim 2, wherein the pickup carriage further includes a moveable cam member disposed on a bottom surface of the pickup carriage.
4. The biopsy device of claim 2, further comprising an actuation lever that is operatively connected to the pickup carriage by a resilient bridge member.
5. The biopsy device of claim 1, wherein the stylet assembly further comprises a first arm sub-assembly that is fixedly attached to the stylet and a second sub-assembly that is movably attached to the stylet.
6. The biopsy device of claim 5, wherein the first arm sub-assembly includes a leg member and a carrier member.
7. The biopsy device of claim 5, wherein the second arm sub-assembly includes a first leg member and a second leg member that are connected together by a carrier member.
8. The biopsy device of claim 1, wherein the vacuum chamber comprises first and second seal members and a cylinder disposed over the first and second seal members; wherein the first seal member is operatively connected to a moveable portion of the stylet assembly and the second seal member is fixedly attached to a portion of the stylet proximal to the first seal member;wherein the stylet further includes a notch that is in communication with the lumen; andwherein the notch is positioned between the first and second seal members.
9. The biopsy device of claim 8, further comprising a vacuum valve that selective covers the notch.
10. The biopsy device of claim 1, further comprising a normally closed valve disposed on a proximal end of the stylet.
11. The biopsy device of claim 10, wherein the normally closed valve further comprises a body and a flap member that selective opens in response to positive pressure.
12. The biopsy device of claim 1, wherein the handpiece further comprises a stylet firing member and an outer cannula firing member, wherein the stylet firing member releases the stylet from a biopsy ready position to a fired position; and wherein the outer cannula firing member releases the outer cannula from a biopsy ready position to a fired position.
13. The biopsy device of claim 12, wherein at least one of the stylet firing member and the outer cannula firing member includes an indicator that differentiates between the stylet firing member and the outer cannula firing member.
14. The biopsy device of claim 1, wherein the handpiece further comprises an indicator that informs a user when the biopsy device is in a biopsy ready position.
15. The biopsy device of claim 1, wherein the outer cannula assembly further comprises an outer cannula hub that is fixedly connected to the outer cannula; wherein the outer cannula hub includes a retaining member that serves to selectively retain the outer cannula assembly in a biopsy ready position within the handpiece.
16. The biopsy device of claim 15, further comprising a support rib, wherein the support rib is slidingly received on the stylet, proximal to the outer cannula hub.
17. The biopsy device of claim 16, wherein a biasing member is positioned between the support rib and the outer cannula hub.
18. The biopsy device of claim 1, further comprising an introducer assembly that is selectively engagable with the biopsy device, wherein the introducer assembly comprises an introducer cannula that is configured to be slidingly disposed over the outer cannula and sized such that a portion of the outer cannula is positioned distally of a distal end of the introducer cannula.
19. The biopsy device of claim 18, wherein the introducer assembly includes a latch member that cooperates with a portion of the handpiece of the biopsy device to selectively fix the introducer cannula to the biopsy device.

CROSS-REFERENCE TO RELATED APPLICATIONS

This application is a Continuation-in-part of U.S. Ser. No. 12/039,364 filed Feb. 28, 2008, which claims priority to U.S. Provisional patent application Ser. No. 60/892,174, filed on Feb. 28, 2007 and which is a Continuation-in-part of U.S. Ser. No. 11/389,274 filed on Mar. 24, 2006, which is a Continuation-in-Part of U.S. Serial No. 10/964,959 filed Oct. 14, 2004 now U.S. Pat. No. 7,390,306 which claims priority to U.S. provisional patent application Ser. No. 60/510,866 filed on Oct. 14, 2003, the disclosures of which are incorporated herein by reference in their entireties. This application also claims benefit of U.S. provisional patent application Ser. No. 60,970,770 filed on Sep. 7, 2007, the contents of which is also incorporated herein by reference in its entirety.

US Referenced Citations (245)

Number	Name	Date	Kind
2472116	Maynes	Jun 1949	A
2660342	Ruf	Nov 1953	A
2735427	Sullivan	Feb 1956	A
2863452	Ogle, Sr.	Dec 1958	A
2892457	Sturtz	Jun 1959	A
3401684	Dremann	Sep 1968	A
3456806	Borston	Jul 1969	A
3477423	Griffith	Nov 1969	A
3517688	Scholle	Jun 1970	A
3561429	Jewett et al.	Feb 1971	A
3815604	O'Malley et al.	Jun 1974	A
3819091	Hollender	Jun 1974	A
3844272	Banko	Oct 1974	A
3889657	Baumgarten	Jun 1975	A
3905365	Colombo	Sep 1975	A
3937222	Banko	Feb 1976	A
3938505	Jamshidi	Feb 1976	A
3945375	Banko	Mar 1976	A
3994297	Kopf	Nov 1976	A
4007742	Banko	Feb 1977	A
D243559	Hoyle et al.	Mar 1977	S
4019514	Banko	Apr 1977	A
4101756	Yamano	Jul 1978	A
4117843	Banko	Oct 1978	A
4159773	Losenno	Jul 1979	A
4167943	Banko	Sep 1979	A
4167944	Banko	Sep 1979	A
4210146	Banko	Jul 1980	A
4257425	Ryan	Mar 1981	A
4301802	Poler	Nov 1981	A
4308878	Silva	Jan 1982	A
4316465	Dotson, Jr.	Feb 1982	A
4354093	Zago	Oct 1982	A
4368734	Banko	Jan 1983	A
4461305	Cibley	Jul 1984	A
4513745	Amoils	Apr 1985	A
4530356	Helfgott et al.	Jul 1985	A
4533818	Green	Aug 1985	A
4549554	Markham	Oct 1985	A
4562838	Walker	Jan 1986	A
4570632	Woods	Feb 1986	A
4594073	Stine	Jun 1986	A
4600014	Beraha	Jul 1986	A
4605011	Naslund	Aug 1986	A
4644951	Bays	Feb 1987	A
4651753	Lifton	Mar 1987	A
4667684	Leigh	May 1987	A
4696298	Higgins et al.	Sep 1987	A
4697600	Cardenas et al.	Oct 1987	A
4699154	Lindgren	Oct 1987	A
4708147	Haaga	Nov 1987	A
4711250	Gilbaugh, Jr. et al.	Dec 1987	A
4733671	Mehl	Mar 1988	A
4735215	Goto et al.	Apr 1988	A
4747414	Brossel	May 1988	A
4776346	Beraha et al.	Oct 1988	A
4776840	Freitas et al.	Oct 1988	A
4781700	Vicario	Nov 1988	A
4803341	Barowski et al.	Feb 1989	A
4817631	Schnepp-Pesch et al.	Apr 1989	A
4850373	Zatloukal et al.	Jul 1989	A
4871074	Bryson et al.	Oct 1989	A
4881551	Taylor	Nov 1989	A
4893635	de Groot et al.	Jan 1990	A
4907598	Bauer	Mar 1990	A
4919146	Rhinehart et al.	Apr 1990	A
4926877	Bookwalter	May 1990	A
RE33258	Onik et al.	Jul 1990	E
4950265	Taylor	Aug 1990	A
4973019	Baird et al.	Nov 1990	A
4982739	Hemstreet et al.	Jan 1991	A
4985027	Dressel	Jan 1991	A
5019036	Stahl	May 1991	A
5025797	Baran	Jun 1991	A
5027827	Cody et al.	Jul 1991	A
5031778	Edgecombe	Jul 1991	A
5048538	Terwilliger et al.	Sep 1991	A
5054615	Stillwagon et al.	Oct 1991	A
5074311	Hasson	Dec 1991	A
5090649	Tipp	Feb 1992	A
5124532	Hafey et al.	Jun 1992	A
5127419	Kaldany	Jul 1992	A
5133360	Spears	Jul 1992	A
5141189	Andrew	Aug 1992	A
D329304	Tipp	Sep 1992	S
5159933	Hut	Nov 1992	A
5172701	Leigh	Dec 1992	A
D332670	McFarland	Jan 1993	S
5183052	Terwilliger	Feb 1993	A
5188118	Terwilliger	Feb 1993	A
5213110	Kedem et al.	May 1993	A
5220926	Jones	Jun 1993	A
5224470	Schnepp-Pesch et al.	Jul 1993	A
5246011	Caillouette	Sep 1993	A
5249582	Taylor	Oct 1993	A
D342585	Fischbach et al.	Dec 1993	S
5275609	Pingleton et al.	Jan 1994	A
5281197	Arias et al.	Jan 1994	A
5282476	Terwilliger	Feb 1994	A
5285795	Ryan et al.	Feb 1994	A
5289831	Bosley	Mar 1994	A
5295890	Myers	Mar 1994	A
5295980	Ersek	Mar 1994	A
5348022	Leight et al.	Sep 1994	A
5400798	Baran	Mar 1995	A
5403276	Schechter et al.	Apr 1995	A
5411513	Ireland et al.	May 1995	A
5423844	Miller	Jun 1995	A
5425376	Banys et al.	Jun 1995	A
5429138	Jamshidi	Jul 1995	A
5456267	Stark	Oct 1995	A
5458112	Weaver	Oct 1995	A
5464300	Crainich	Nov 1995	A
5469860	De Santis	Nov 1995	A
5492130	Chiou	Feb 1996	A
5505211	Ohto et al.	Apr 1996	A
5511556	DeSantis	Apr 1996	A
5520635	Gelbfish	May 1996	A
D371220	Behrens	Jun 1996	S
5526822	Burbank et al.	Jun 1996	A
5535755	Heske	Jul 1996	A
5546957	Heske	Aug 1996	A
5560373	De Santis	Oct 1996	A
5575293	Miller et al.	Nov 1996	A
5580347	Reimels	Dec 1996	A
D377996	Gilbert	Feb 1997	S
5615782	Choe	Apr 1997	A
D379554	Landers	May 1997	S
5643304	Schechter et al.	Jul 1997	A
5649547	Ritchart et al.	Jul 1997	A
5669876	Schechter et al.	Sep 1997	A
5669923	Gordon	Sep 1997	A
D386818	Boomfield	Nov 1997	S
5685840	Schechter et al.	Nov 1997	A
5730717	Gelbfish	Mar 1998	A
5769086	Ritchart et al.	Jun 1998	A
5775333	Burbank et al.	Jul 1998	A
5782849	Miller	Jul 1998	A
5788651	Weilandt	Aug 1998	A
5794626	Kieturakis	Aug 1998	A
5794799	Collins et al.	Aug 1998	A
5797907	Clement	Aug 1998	A
5810806	Ritchart et al.	Sep 1998	A
5817033	DeSantis et al.	Oct 1998	A
5843111	Vijfvinkel	Dec 1998	A
5848978	Cecchi	Dec 1998	A
D403810	Owens	Jan 1999	S
5893862	Pratt et al.	Apr 1999	A
5911701	Miller et al.	Jun 1999	A
5913857	Ritchart et al.	Jun 1999	A
5916229	Evans	Jun 1999	A
5928164	Burbank et al.	Jul 1999	A
5928218	Gelbfish	Jul 1999	A
5944673	Gregoire et al.	Aug 1999	A
5964716	Gregoire et al.	Oct 1999	A
5971939	DeSantis et al.	Oct 1999	A
5980469	Burbank et al.	Nov 1999	A
5980545	Pacala et al.	Nov 1999	A
5980546	Hood	Nov 1999	A
5993399	Pruitt et al.	Nov 1999	A
5997560	Miller	Dec 1999	A
6007497	Huitema	Dec 1999	A
6017316	Ritchart et al.	Jan 2000	A
6019733	Farascioni	Feb 2000	A
6022324	Skinner	Feb 2000	A
D423717	Taylor	Apr 2000	S
6050955	Bryan et al.	Apr 2000	A
D426025	Holmes et al.	May 2000	S
6059807	Boudjema	May 2000	A
6077230	Gregoire et al.	Jun 2000	A
6080113	Heneveld et al.	Jun 2000	A
6085749	Wardle et al.	Jul 2000	A
6086544	Hibner et al.	Jul 2000	A
6096042	Herbert	Aug 2000	A
6109446	Foote	Aug 2000	A
6120462	Hibner et al.	Sep 2000	A
6120463	Bauer	Sep 2000	A
6123299	Zach, Sr.	Sep 2000	A
6142955	Farascioni et al.	Nov 2000	A
6155989	Collins	Dec 2000	A
6161034	Burbank et al.	Dec 2000	A
6162187	Buzzard et al.	Dec 2000	A
6193414	Balzano	Feb 2001	B1
6193673	Viola et al.	Feb 2001	B1
6251418	Ahern et al.	Jun 2001	B1
6258064	Smith et al.	Jul 2001	B1
6273862	Privitera et al.	Aug 2001	B1
6280399	Rossin et al.	Aug 2001	B1
6293957	Peters et al.	Sep 2001	B1
6346107	Cucin	Feb 2002	B1
6347241	Burbank et al.	Feb 2002	B2
6358217	Bourassa	Mar 2002	B1
6387057	Heske	May 2002	B1
6402701	Kaplan et al.	Jun 2002	B1
6428486	Ritchart et al.	Aug 2002	B2
6436054	Viola et al.	Aug 2002	B1
6461350	Underwood et al.	Oct 2002	B1
6468225	Lundgren	Oct 2002	B1
6468227	Zimmon	Oct 2002	B2
6485436	Truckai et al.	Nov 2002	B1
6488636	Bryan et al.	Dec 2002	B2
6494844	Van Bladel et al.	Dec 2002	B1
6506165	Sweeney	Jan 2003	B1
6514215	Ouchi	Feb 2003	B1
6551255	Van Bladel et al.	Apr 2003	B2
6554778	Fleming, III	Apr 2003	B1
6554779	Viola et al.	Apr 2003	B2
6572563	Ouchi	Jun 2003	B2
6589240	Hinchliffe	Jul 2003	B2
6592530	Farhadi	Jul 2003	B1
6626868	Prestidge et al.	Sep 2003	B1
6632182	Treat	Oct 2003	B1
6702760	Krause et al.	Mar 2004	B2
6712773	Viola	Mar 2004	B1
6725083	Burbank et al.	Apr 2004	B1
6863676	Lee et al.	Mar 2005	B2
6942627	Huitema	Sep 2005	B2
6997926	Gellman et al.	Feb 2006	B2
7278970	Goldenberg	Oct 2007	B2
7390306	Mark	Jun 2008	B2
7608048	Goldenberg	Oct 2009	B2
20010014785	Sussman et al.	Aug 2001	A1
20020111563	Hall	Aug 2002	A1
20030018281	Huitema	Jan 2003	A1
20030125639	Fisher et al.	Jul 2003	A1
20030153874	Tal	Aug 2003	A1
20030195436	Van Bladel et al.	Oct 2003	A1
20030229293	Hibner et al.	Dec 2003	A1
20040097830	Cooke et al.	May 2004	A1
20040158172	Hancock	Aug 2004	A1
20040162572	Sauer	Aug 2004	A1
20040230133	Miller et al.	Nov 2004	A1
20050027210	Miller	Feb 2005	A1
20050054947	Goldenberg	Mar 2005	A1
20050075580	Leigh et al.	Apr 2005	A1
20050080355	Mark	Apr 2005	A1
20050203439	Heske et al.	Sep 2005	A1
20050240118	Huitema	Oct 2005	A1
20050277829	Tsonton et al.	Dec 2005	A1
20060089565	Schramm	Apr 2006	A1
20060155210	Beckman et al.	Jul 2006	A1
20060173377	McCullough et al.	Aug 2006	A1
20070106176	Mark et al.	May 2007	A1
20080200835	Monson et al.	Aug 2008	A1
20090204023	Goldenberg	Aug 2009	A1

Foreign Referenced Citations (17)

Number	Date	Country
1551362	Jan 1987	CH
1160573	Jan 1964	DE
141 108	Apr 1980	DE
20204363	May 2002	DE
0 010 321	Apr 1980	EP
0561732	Sep 1993	EP
1520518	Apr 2005	EP
1 698 283	Sep 2006	EP
WO-8303343	Oct 1983	WO
WO-9624289	Aug 1996	WO
WO-9720504	Jun 1997	WO
WO-0222023	Mar 2002	WO
WO-03009766	Feb 2003	WO
WO-2005037106	Apr 2005	WO
WO-2005063126	Jul 2005	WO
WO-2006083770	Aug 2006	WO
WO-2008106583	Sep 2008	WO

Related Publications (1)

	Number	Date	Country
	20090082696 A1	Mar 2009	US

Provisional Applications (3)

Number	Date	Country
60892174	Feb 2007	US
60510866	Oct 2003	US
60970770	Sep 2007	US

Continuation in Parts (4)

	Number	Date	Country
Parent	12039364	Feb 2008	US
Child	12205291		US
Parent	11389274	Mar 2006	US
Child	12039364		US
Parent	10964959	Oct 2004	US
Child	11389274		US
Parent	12205291		US
Child	11389274		US

Vacuum assisted biopsy device

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