Patent Grant
11241296
The disclosure relates generally to tissue markers. More particularly, the disclosure relates to implantable tissue markers for use in magnetic resonance imaging.
Certain medical conditions, including breast cancer, are increasingly being diagnosed and treated using minimally invasive medical techniques. Such techniques typically involve the use of clinical imaging methods that allow the physician to visualize interior portions of a patient's body without the need to make excessive incisions or cause avoidable collateral damage to healthy adjacent tissue. Imaging can be performed using any of variety of modalities, including, for example, X-rays, computed tomographic (CT) X-ray imaging, fluoroscopy, portal film imaging devices, electronic portal imaging devices, ultrasound, electrical impedance tomography (EIT), magnetic resonance (MR) imaging, or MRI, magnetic source imaging (MSI), magnetic resonance spectroscopy (MRS), magnetic resonance mammography (MRM), magnetic resonance angiography (MRA), magnetoelectro-encephalography (MEG), laser optical imaging, electric potential tomography (EPT), brain electrical activity mapping (BEAM), arterial contrast injection angiography, and digital subtraction angiography. Nuclear medicine modalities include positron emission tomography (PET) and single photon emission computed tomography (SPECT).
Some of these imaging procedures involve the use of radiographic markers. Radiographic markers are small devices that are implanted in a patient during surgical procedures, such as biopsies. Conventional markers typically consist of one or more solid objects, such as a piece of metallic wire, ceramic beads, etc., which are implanted either by themselves or within a gelatinous matrix, collagen, or polylactic acid, to temporarily increase visibility, for example, to ultrasound imaging. They are designed to be visible to one of the imaging modalities listed above and typically have a shape that is readily identifiable as an artificial structure, as contrasted from naturally occurring anatomical structures in the patient's body. For example, markers can be shaped as coils, stars, rectangles, spheres, or other shapes that do not occur in anatomical structures. Such markers enable radiologists to localize the site of surgery in subsequent imaging studies or to facilitate image registration during image-guided therapeutic procedures. In this way, markers can serve as landmarks that provide a frame of reference for the radiologist.
Most conventional markers appear as a signal void, i.e., a dark artifact, in magnetic resonance imaging. This manifestation can be particularly problematic in some contexts. For example, heterogeneous breast tissue produces many dark artifacts under MR imaging, thereby rendering small signal voids produced by some conventional markers difficult to identify and distinguish from naturally occurring dark artifacts. In addition, some markers produce large susceptibility artifacts under MR imaging, thereby distorting images in both MRI and spectroscopic modalities. Some markers incorporate an external gel that may produce a positive or bright signal, but such gels are not permanent. Some other markers contain collagen or polylactic acid, which may interfere with magnetic resonance spectroscopy. With the increasing use of MR imaging techniques in the treatment of breast cancer in clinical settings, improved MR visibility of tissue markers is particularly desirable.
According to various example embodiments, an implantable tissue marker incorporates a contrast agent sealed within a chamber in a container formed from a solid material. The contrast agent is selected to produce a change in signal intensity under magnetic resonance imaging (MRI). An additional contrast agent may also be sealed within the chamber to provide visibility under another imaging modality, such as computed tomographic (CT) imaging or ultrasound imaging.
One embodiment is directed to a permanently implantable radiographic marker. A container formed from a solid material defines an internal chamber, in which a contrast agent is sealed. The contrast agent is selected to produce an increase in signal intensity in a magnetic resonance (MR) imaging modality. Another embodiment is directed to a method of manufacturing such a marker.
In another embodiment, a permanently implantable fiducial marker includes a container formed from a nonbiodegradable solid material. The container defines an internal chamber. A first contrast agent is sealed within the internal chamber and is selected to produce an increase in signal intensity in a magnetic resonance (MR) imaging modality. A second contrast agent sealed within the internal chamber. The second contrast agent is selected to produce a signal in another imaging modality.
Another embodiment is directed to a method of identifying a location within a body of a patient. A marker is implanted proximate the location. The marker comprises a container formed from a solid material and defining an internal chamber, and a contrast agent sealed within the internal chamber. The contrast agent is selected to produce an increase in signal intensity in a magnetic resonance (MR) imaging modality. A first image of the location is generated in the magnetic resonance (MR) imaging modality.
Various embodiments may provide certain advantages. For instance, a contrast agent selected to produce an increase in signal intensity in an MR imaging modality may produce good visualization characteristics without also producing an excessive artifact and without interfering with MR spectroscopy or diffusion imaging. Production of an increase in signal intensity in an MR imaging modality may be particularly beneficial in certain contexts, such as, for example, imaging of breast tissue, which is heterogeneous.
Additional objects, advantages, and features will become apparent from the following description and the claims that follow, considered in conjunction with the accompanying drawings.
This overview is intended to provide an overview of subject matter of the present patent application. It is not intended to provide an exclusive or exhaustive explanation of the present subject matter. The detailed description is included to provide further information about the present patent application.
In the drawings, which are not necessarily drawn to scale, like numerals may describe similar components in different views. Like numerals having different letter suffixes may represent different instances of similar components. The drawings illustrate generally, by way of example, but not by way of limitation, various embodiments discussed in the present document.
According to various embodiments, an implantable tissue marker incorporates a contrast agent sealed within a chamber in a container formed from a solid material. The contrast agent is selected to produce an increase in signal intensity under magnetic resonance imaging (MRI). An additional contrast agent may also be sealed within the chamber to provide visibility under another imaging modality, such as computed tomographic (CT) imaging or ultrasound imaging.
In this way, certain advantages may be realized. For instance, a contrast agent selected to produce an increase in signal intensity in an MR imaging modality may produce good visualization characteristics without also producing an excessive artifact and without interfering with MR spectroscopy or diffusion imaging. Producing an increase in signal intensity in an MR imaging modality may be particularly beneficial in certain contexts, such as, for example, imaging of breast tissue. Most conventional markers appear as a signal void in MR imaging. The heterogeneous nature of breast tissue makes small signal voids difficult to identify. By producing an increase in signal intensity, i.e., a bright area, in MR imaging, the implantable tissue markers disclosed herein may be easier to see than conventional markers.
The following description of various embodiments implemented in the context of imaging certain types of tissue is to be construed by way of illustration rather than limitation. This description is not intended to limit the invention or its applications or uses. For example, while various embodiments are described as being implemented in the context of imaging breast tissue, it will be appreciated that the principles of the disclosure are applicable to other contexts, such as image registration during image guided therapeutic procedures. In further examples, while various embodiments are described as being implemented in the context of imaging breast tissue, it will be appreciated that the principles of the disclosure are applicable to other anatomical sites, such as prostate, brain, spinal, and other anatomical sites.
In the following description, numerous specific details are set forth in order to provide a thorough understanding of various embodiments. It will be apparent to one skilled in the art that some embodiments may be practiced without some or all of these specific details. In other instances, well known components and process steps have not been described in detail.
Referring now to the drawings,
The tube 102 defines two end portions 104 and 106, at least one of which is initially open. A chamber 108 is defined within the tube 102 between the two end portions 104 and 106. One or more contrast agents 110 are introduced into the chamber 108. The end portions 104 and 106 are then sealed, for example, using a sealant 112 such as epoxy. In some embodiments, a permanent biocompatible adhesive such as cyanoacrylate serves as the sealant 112.
The visual representation of the contrast agents 110 in
For instance, if the marker 100 is to be visible in magnetic resonance (MR) and computed tomographic (CT) imaging modalities, the chamber 108 may contain a mixture of a gadolinium-DTPA MR contrast agent and an iodinated CT contrast agent. The volume of contrast agent 110 in the chamber 108 may be maximized to promote visibility. Visibility is also promoted by matching the magnetic susceptibility of the contrast agent 110 and the magnetic susceptibility of the tube 102. If it is further desired that the marker 100 be visible in an ultrasound imaging modality, the chamber 108 may also contain a gas bubble.
In some embodiments, the tube 102 itself, rather than multiple contrast agents 110, may provide visibility in certain imaging modalities. For example, the tube 102 may be made of a radiopaque polymer that provides contrast in X-ray imaging modalities. As another example, a difference in acoustic impedance between the tube 102 and the material in the chamber 108 will cause the marker 100 to reflect ultrasound waves, thereby promoting visibility in an ultrasound imaging modality. Further, if the magnetic susceptibility of the tube 102 is similar to that of the material in the chamber 108 and to that of the surrounding tissue, visibility in MR imaging modalities will be improved due to improved magnetic field homogeneity and reduced T2*artifact.
In one particular embodiment, the marker 100 is formed by cutting a glass micropipette, commercially available from Fisher Scientific, headquartered in Hampton, N.H., to the desired length, e.g., 4 mm, to form the tube 102. The micropipette has an outer diameter appropriate for insertion via a biopsy cannula, e.g., 2 mm.
Contrast agents 110 are then introduced into the chamber 108 defined by the tube 102. In one particular embodiment, for example, an MR contrast agent and a CT contrast agent are combined, and the liquid mixture resulting from this combination is injected into the micropipette via a syringe of appropriate gauge, e.g., 25 ga. The MR contrast agent may be implemented as a gadolinium-based MR contrast agent, such as MAGNEVIST® MR contrast agent, commercially available from Berlex, headquartered in Montville, N.J. Other MR contrast agents include, but are not limited to, OMNISCAN™ MR contrast agent, commercially available from GE Healthcare, headquartered in Chalfont St. Giles, United Kingdom, PROHANCE® MR contrast agent, and OPTIMARK® MR contrast agent, commercially available from Tyco Healthcare/Mallinckrodt, Inc., headquartered in St. Louis, Mo. The CT contrast agent may be implemented as an iodinated CT contrast agent, such as OMNIPAQUE™ CT contrast agent, commercially available from GE Healthcare, headquartered in Chalfont St. Giles, United Kingdom. Other CT contrast agents include, but are not limited to, HEXABRIX®, TELEBRIX®, and CONRAY® CT contrast agents, commercially available from Tyco Healthcare/Mallinckrodt, Inc., headquartered in St. Louis, Mo. After the mixture is injected in the chamber 108, the ends of the tube 102 are sealed using a quick-setting epoxy.
Markers 100 of the type illustrated in
The evaluation of the markers 100 demonstrated that the markers 100 were clearly visible on the three modalities, namely, MRI, X-ray mammography, and ultrasound.
In addition to the MRI modality, the markers 100 were also visible in the X-ray mammography and ultrasound imaging modalities. In the X-ray mammography modality, the radiopaque liquid occupying the chamber 108 could be seen clearly with distinct edges. In the ultrasound modality, the tube 102 appeared hyperechoic, while the contrast agents 110 occupying the chamber 108 appeared dark. In this modality, the markers 100 were most easily seen when they were oriented parallel to the transducer surface. However, the markers 100 could also be detected when they were oriented perpendicular to the transducer surface.
According to various embodiments, the contrast agents 110 that are sealed within the chamber 108 can be selected for visibility in any of a number of imaging modalities. Besides the MR, X-ray, and ultrasound imaging modalities mentioned above, contrast agents can be selected for visibility in computed tomographic (CT) X-ray imaging, fluoroscopy, portal film imaging, electronic portal imaging, electrical impedance tomography (EIT), magnetic source imaging (MSI), magnetic resonance spectroscopy (MRS), magnetic resonance mammography (MRM), magnetic resonance angiography (MRA), magnetoelectro-encephalography (MEG), laser optical imaging, electric potential tomography (EPT), brain electrical activity mapping (BEAM), arterial contrast injection angiography, and digital subtraction angiography modalities. Nuclear medicine modalities include positron emission tomography (PET) and single photon emission computed tomography (SPECT). In addition, as additional imaging modalities are developed in the future, it will be possible to seal contrast agents within the chamber 108 that are selected for visibility in such future modalities.
One or more contrast agents 126 are introduced into the chamber 124, for example, by injecting the contrast agents 126 into the chamber 124. The visual representation of the contrast agents 126 in
In some embodiments, the capsule 122 itself, rather than multiple contrast agents 126, may provide visibility in certain imaging modalities. For example, the capsule 122 may be made of a radiopaque polymer that provides contrast in X-ray imaging modalities. As another example, a difference in acoustic impedance between the capsule 122 and the material in the chamber 124 will cause the marker 120 to reflect ultrasound waves, thereby promoting visibility in an ultrasound imaging modality. Further, if the magnetic susceptibility of the capsule 122 is similar to that of the material in the chamber 124 and to that of the surrounding tissue, visibility in MR imaging modalities will be improved due to reduction of T2 darkening.
One or more contrast agents 136 are introduced into the chamber 134, for example, by injecting the contrast agents 136 into the chamber 134. The visual representation of the contrast agents 136 in
In some embodiments, the capsule 132 itself, rather than multiple contrast agents 136, may provide visibility in certain imaging modalities. For example, the capsule 132 may be made of a radiopaque polymer that provides contrast in X-ray imaging modalities. As another example, a difference in acoustic impedance between the capsule 132 and the material in the chamber 134 will cause the marker 130 to reflect ultrasound waves, thereby promoting visibility in an ultrasound imaging modality. Further, if the magnetic susceptibility of the capsule 132 is similar to that of the material in the chamber 134 and to that of the surrounding tissue, visibility in MR imaging modalities will be improved due to reduction of T2 darkening.
The markers 100, 120, and 130 illustrated in
An image of the location is then generated in an MRI modality. In addition, another image of the location can be generated in another imaging modality, such as a CT X-ray imaging modality. Other imaging modalities may be employed, such as ultrasound, X-ray, fluoroscopy, electrical impedance tomography, magnetic source imaging (MSI), magnetic resonance spectroscopy (MRS), magnetic resonance mammography (MRM), magnetic resonance angiography (MRA), magnetoelectroencephalography (MEG), laser optical imaging, electric potential tomography (EPT), brain electrical activity mapping (BEAM), arterial contrast injection angiography, digital subtraction angiography, positron emission tomography (PET), and single photon emission computed tomography (SPECT).
If multiple imaging modalities are employed, positional information for the area of the body that was imaged can be determined as a function of the images thus generated. For example, the images can be registered so as to align the coordinate systems of the images. In this way, any point in the imaged area of the body is made to correspond to identical addresses in each image. This registration process involves the use of rigid body transformation techniques, which in three-dimensional images requires knowledge of at least three points in each image. The markers described above may serve as fiducial markers to mark these points in the images. Accordingly, the fiducial markers can be used to correlate the spaces in each image, both with respect to physical space and with respect to the other images. In addition, the fiducial markers provide a constant frame of reference that is visible in each imaging modality to facilitate registration.
As demonstrated by the foregoing discussion, various embodiments may provide certain advantages, particularly in the context of imaging heterogeneous breast tissue. For instance, the use of a mixture of an MR contrast agent and a CT contrast agent may promote visibility in multiple imaging modalities, thus facilitating registering images obtained by multimodal imaging procedures. A contrast agent selected to produce an increase in signal intensity in an MR imaging modality may produce good visualization characteristics without also producing an excessive artifact and without interfering with MR spectroscopy or diffusion imaging. By producing an increase in signal intensity in MR imaging, the implantable tissue markers disclosed herein may be easier to see than conventional markers.
Because the contrast agents are sealed within the tube or capsule, they are at least substantially permanent and are not absorbed by the patient's body. Thus, multimodal imaging using the markers disclosed herein also allows a clinician to monitor an anatomical site over a period of time using images from multiple modalities, if desired. If the anatomical site in question requires treatment, the markers can be used to determine the precise location of the anatomical site and thus guide therapy. For example, markers can be implanted at a lesion site prior to removing the lesion to guide the procedure. After the lesion is removed, the markers can be used to monitor the site overtime.
It will be understood by those who practice the embodiments described herein and those skilled in the art that various modifications and improvements may be made without departing from the spirit and scope of the disclosed embodiments. For example, the markers disclosed herein may incorporate therapeutic agents, such as radioactive agents, anti-inflammatory agents, anti-microbial agents, hemostatic agents, biocompatible adhesives, proteins, stem cells, or other material. Such agents may be applied to an external surface of the markers or disposed within the internal chambers. Accordingly, the scope of protection afforded is to be determined solely by the claims and by the breadth of interpretation allowed by law.
Referring to
Referring to
In some examples, one or more contrast agents 210 are introduced into the chamber 208. The opening 203, in an example, is sealed with the lid portion 204 to seal the contrast agent 210 within the chamber 208, in some examples, the opening 203 can be sealed in various ways, including press-fitting the lid portion 204 within the opening 203 of the container 202, using sealant or epoxy, or using other sealing techniques, such as, for instance ultrasonic welding of the lid portion 204 and the container 202. The visual representation of the contrast agents 210 in
In an example, the marker 200 is formed by injection molding the container 202 and the lid portion 204. In another example, the marker 200 can be formed by micromachining. In a further example, the marker 200 can be encapsulated by a material, such as, for instance, silicone, PTFE, or another substance capable of performing as described herein. Such encapsulation, in various examples, can improve the seal of the marker 200; improve the bio-compatibility of the marker 200; can improve the surface properties of the marker 200, for instance, to facilitate deployment of the marker 200 through trocar or other device; or reduce bio-mobility of the marker 200 once it is implanted.
Referring to
In some examples, one or more contrast agents 310 are introduced into the chamber 308. The openings 303, in an example, are sealed with the lid portions 304, 306 to seal the contrast agent 310 within the chamber 308. In some examples, the openings 303, 305 can be sealed in various ways, including press-fitting the lid portions 304, 306 within the openings 303, 305 of the container 302, using sealant or epoxy, or using other sealing techniques, such as, for instance ultrasonic welding of the lid portions 304, 306 and the container 302. The visual representation of the contrast agents 310 in
In an example, the marker 300 is formed by injection molding the container 302 and the lid portions 304, 306. In another example, the marker 300 can be formed by micromachining. In a further example, the marker 300 can be encapsulated by a material, such as, for instance, silicone, PTFE, or another substance capable of performing as described herein. Such encapsulation, in various examples, can improve the seal of the marker 300; improve the bio-compatibility of the marker 300; can improve the surface properties of the marker 300, for instance, to facilitate deployment of the marker 300 through trocar or other device; or reduce bio-mobility of the marker 300 once it is implanted.
With reference to
In several examples, the method includes at least partially filling the internal chamber 108, 124, 134, 208, 308 with the contrast agent 110, 126, 136, 210, 310. Such filling can be accomplished in various manners including, but not limited to those described herein. In an example, the container 102, 122, 132, 202, 302 can be immersed within the contrast agent 110, 126, 136, 210, 310 to inhibit gas from being sealed within the internal chamber 108, 124, 134, 208, 308 in a further example, the container 102, 122, 132, 202, 302 is sealed while the container 102, 122, 132, 202, 302 is immersed in the contrast agent 110, 126, 136, 210, 310 to further inhibit unwanted materials from being sealed within the internal chamber 108, 124, 134, 208, 308 of the container 102, 122, 132, 202, 302. In an example, the container 102, 122, 132, 202, 302 can be immersed within a vat, receptacle, tank, etc. of the contrast agent 110, 126, 136, 210, 310 in order to lessen the amount of air or another gas from being present within the internal chamber 108, 124, 134, 208, 308 prior to sealing of the container 102, 122, 132, 202, 302. In some examples, the internal chamber 108, 124, 134, 208, 308 is at least partially filled with the contrast agent 110, 126, 136, 210, 310 with the container 102, 122, 132, 202, 302 within a chamber filled with a gas other than ambient air to inhibit ambient air from being sealed within the internal chamber 108, 124, 134, 208, 308. In an example, the chamber within which the container 102, 122, 132, 202, 302 is filled includes air or another gas at a pressure other than ambient pressure. For instance, the container 102, 122, 132, 202, 302 can be filled in a vacuum, in a high pressure environment, or in a pressure therebetween in some examples, the internal chamber 108, 124, 134, 208, 308 can be filled with the contrast agent 110, 126, 136, 210, 310 with the container 102, 122, 132, 202, 302 within a chamber substantially filled with a gas other than air. In a further example, the internal chamber 108, 124, 134, 208, 308 can be filled with the container 102, 122, 132, 202, 302 within the chamber substantially filled with nitrogen. For instance, in certain examples, oxygen (present in air) can be undesirable due to magnetic properties that could make susceptibility matching of the marker 100, 120, 130, 200, 300 more difficult than if oxygen were not present. In this example, filling of the container 102, 122, 132, 202, 302 with the contrast agent 110, 126, 136, 210, 310 within a nitrogen-filled chamber would cause residual gas bubbles within the container 102, 122, 132, 202, 302 to be nitrogen rather than oxygen, which can be more desirable in certain examples due to the different magnetic properties of nitrogen than those of oxygen. However, in other examples, the presence of oxygen within the container 102, 122, 132, 202, 302 can be desirable. In these examples, by adjusting the mixture of air or other gas or gases, the magnetic susceptibility and, therefore, the MRI visibility, of the marker 100, 120, 130, 200, 300 can be adjusted.
In some examples, the container 102, 122, 132, 202, 302 is vibrated during filling to aid in removal of gas bubbles from within the internal chamber 108, 124, 134, 208, 308 prior to sealing of the container 102, 122, 132, 202, 302. Such vibration can cause gas bubbles within the contrast agent 110, 126, 136, 210, 310 to rise out of the contrast agent 110, 126, 136, 210, 310 and toward an opening in the container 102, 122, 132, 202, 302, so that the gas bubbles can exit the container 102, 122, 132, 202, 302 prior to sealing of the container 102, 122, 132, 202, 302. In an example, the container 102, 122, 132, 202, 302 is ultrasonically vibrated in order to aid in removal of gas bubbles from within the internal chamber 108, 124, 134, 208, 308 prior to sealing of the container 102, 122, 132, 202, 302.
The various examples of filling of the container 102, 122, 132, 202, 302 described herein can be used to introduce or decrease amounts of various contrast agent materials within the internal chamber 108, 124, 134, 208, 308 of the container 102, 122, 132, 202, 302, based upon the desired mix of the contrast agent, the desired purity of the contrast agent, the desired response of the contrast agent in various imaging modalities, or the like. In this way, the filling environment and/or the contrast agent 110, 126, 136, 210, 310 within the container 102, 122, 132, 202, 302 can be controlled to tune the response of the marker 100, 120, 130, 200, 300 in one or more of various imaging modalities. The described examples of filling of the container 102, 122, 132, 202, 302 are meant to be illustrative and are not intended to be limiting. As such, additional techniques and methods of filling the container 102, 122, 132, 202, 302 are contemplated herein.
In some examples, the method includes mixing a first contrast agent configured to produce the change in signal intensity in the MR imaging modality and a second contrast agent configured to produce a signal in another imaging modality. In an example, the other imaging modality includes a computed tomographic (CT) X-ray imaging modality. In other examples, the other imaging modality includes one of an ultrasound imaging modality, an X-ray imaging modality, a fluoroscopy imaging modality, an electrical impedance tomographic imaging modality, a magnetic source imaging (MSI) modality, an magnetic resonance spectroscopic (MRS) modality, a magnetic resonance mammographic (MRM) modality, a magnetic resonance angiographic (MRA) modality, a magnetoelectroencephalographic (MEG) modality, a laser optical imaging modality, an electric potential tomographic (EPT) modality, a brain electrical activity mapping (BEAM) modality, an arterial contrast injection angiographic modality, a digital subtraction angiographic modality, a positron emission tomographic (PET) modality, and a single photon emission computed tomographic (SPECT) modality. In an example, the contrast agent 110, 126, 136, 210, 310 includes the mixture of the first and second contrast agents. In this example, the mixture of the first and second contrast agents is sealed within the internal chamber 108, 124, 134, 208, 308. In other examples, any number of contrast agents can be mixed together, depending upon the application for which the marker 100, 120, 130, 200, 300 is to be used. In an example, the first contrast agent includes a paramagnetic material. In another example, the first contrast agent includes gadolinium. In a further example, the second contrast agent includes iodine. In various examples, the contrast agent 110, 126, 136, 210, 310 includes at least one of a gas material, a liquid material, or a gel material.
In another example, the method includes sealing a therapeutic agent within the internal chamber 108, 124, 134, 208, 308.
In an example, the method includes forming the container 102, 122, 132, 202, 302 from a solid material configured to produce a signal in an imaging modality other than MR, including, but not limited to other imaging modalities described herein.
In various examples, the method includes forming the container 102, 122, 132, 202, 302 in various ways. In an example, the container 102, 122, 132, 202, 302 is molded. In a further example, the container 102, 122, 132, 202, 302 is injection molded. In a still further example, the container 102, 122, 132, 202, 302 is micromachined. The above examples are intended to be illustrative, not limiting, as it is contemplated that the container 102, 122, 132, 202, 302 can be formed in manners or using techniques other than those described herein, depending upon factors including the materials, size, shape, etc. of the marker 100, 120, 130, 200, 300.
In such examples, the container 102, 122, 132, 202, 302 can be formed from various materials. In some examples, the container 102, 122, 132, 202, 302 is formed from a polymeric material. In a further example, the container 102, 122, 132, 202, 302 is formed from a polyether material. In still further examples, the container 102, 122, 132, 202, 302 is formed from a material including at least one of polytetrafluoroethylene (PTFE), polyether ether ketone (PEEK), polysulfone, polyurethane, and polyethylene. In another example, the container 102, 122, 132, 202, 302 is formed from a silicone-based material. The above examples are intended to be illustrative, not limiting, as it is contemplated that the container 102, 122, 132, 202, 302 can be formed from materials other than those described herein, depending upon the use and desired properties of the marker 100, 120, 130, 200, 300.
In some examples, the method includes forming the tube 102 defining the first and second end portions 104, 106. In an example, the contrast agent 110 is sealed within the internal chamber 108 includes at least substantially sealing the first and second end portions 104, 106 using the biocompatible adhesive 112. In further examples, the tube 102 is formed from a solid material including at least one of a glass material, a ceramic material, a polymer material, silicone, or carbon fiber.
In some examples, the method includes forming a vial-shaped portion 202 of the container 202. In this example, the vial-shaped portion 202 includes the opening 203. In an example, the lid portion 204 of the container 202 is also formed. In this example, the lid portion 204 of the container 202 is configured to be attached at the opening 203 of the vial-shaped portion 202 of the container 202.
In some examples, the method includes forming a first portion 302 including at least two openings 303, 305. In this example, second and third portions 304, 306 are formed and are configured to be attached to the first portion 302 at the at least two openings 303, 305. In an example, the first portion 302 is substantially tube-shaped. In an example, the second and third portions 304, 306 are attached at the respective openings 303, 305 of the first portion 302 to seal the contrast agent 310 within the internal chamber 308. In other examples, the first portion includes other shapes, such as, but not limited to, substantially spherical, substantially ellipsoidal, substantially prismatic, etc. In other examples, the first portion can include more or less than two openings.
In some examples, the method includes coating the marker 100, 120, 130, 200, 300 to encapsulate the marker 100, 120, 130, 200, 300. In an example, the marker 100, 120, 130, 200, 300 is fully encapsulated with a material to improve the seal of the marker 100, 120, 130, 200, 300; improve the bio-compatibility of the marker 100, 120, 130, 200, 300; can improve the surface properties of the marker 100, 120, 130, 200, 300, for instance, to facilitate deployment of the marker 100, 120, 130, 200, 300 through trocar or other device; or reduce bio-mobility of the marker 100, 120, 130, 200, 300 once it is implanted. In an example, such encapsulation hermetically seals the marker 100, 120, 130, 200, 300. Various materials are contemplated for encapsulating the marker 100, 120, 130, 200, 300. For instance, in some examples, the marker 100, 120, 130, 200, 300 can be coated with a material including at least one of silicone or PTFE.
Referring to
In at least one example, the sensing mediums can include a contrast agent 410 as illustrated in
As illustrated in
In an example, the sensor can comprise a sensor such as electrochemical or electronic sensors for monitoring at least one physiological condition. The sensor can have a transmitter for conveying the measured information to an external receiver. In an example, the sensor can have at least one of a passive radio frequency transmitter or a transponder. The physiological condition can comprise at least one of temperature, pH, tissue oxygen levels, and other physiological factors that may be indicative of metabolic function or specific disease state or suggestive of tumor necrosis, angiogenesis, and other biological processes, in this configuration, the outer wall 402 or a portion thereof adjacent to the first or second sub-chamber 409A, 409B containing the sensor can be permeable to permit physiological fluid to enter the first or second sub-chamber 409A, 409B to interact with the sensor.
In an example, the secondary component 411 can comprise structures or transponders such as REED microchips, uniquely shaped solid objects detectable under x-ray imaging modalities, and other identifying components that can be detected and identified by external imaging modalities.
In an example, the outer wall 402 can define a first opening 403 for accessing the first sub-chamber 409A. In this configuration, the marker 400 can include a first lid 413A for enclosing the first sub-chamber 409A. The secondary component or the sensing medium can be sealed in the second sub-chamber 409B. As illustrated in
Example 1 is a permanently implantable radiographic marker, comprising: a biocompatible container having an outer wall defining an internal chamber and an internal wall positioned within the internal chamber to divide the internal chamber into a first sub-chamber and a second sub-chamber; a sensing medium positioned within the first sub-chamber; and a secondary component positioned within the second sub-chamber.
In Example 2, the subject matter of Example 1 optionally includes wherein the biocompatible container further comprises: a second internal wall positioned within the internal chamber to further divide the internal chamber into a plurality of sub-chambers.
In Example 3, the subject matter of any one or more of Examples 1-2 optionally include wherein the sensing medium is detectable by an imaging modality comprising at least one of MRI, ultrasound, x-ray, nuclear machine, infrared, fluorescence, and combinations thereof.
In Example 4, the subject matter of any one or more of Examples 1-3 optionally include wherein the secondary component comprises a sensor for measuring at least one physiological condition.
In Example 5, the subject matter of Example 4 optionally includes wherein the sensor is electrochemical; wherein at least a portion of the outer wall adjacent the second sub-chamber is permeable to permit at least one physiological fluid to permeate into the second sub-chamber.
In Example 6, the subject matter of any one or more of Examples 4-5 optionally include wherein the sensor is electronic.
In Example 7, the subject matter of any one or more of Examples 4-6 optionally include wherein the secondary component further comprises a transmitter for communicating measured physiological conditions.
In Example 8, the subject matter of any one or more of Examples 4-7 optionally include wherein the physiological condition comprises at least one of temperature, pH, and tissue oxygen levels.
In Example 9, the subject matter of any one or more of Examples 1-8 optionally include wherein the secondary component comprises a therapeutic composition.
In Example 10, the subject matter of Example undefined optionally includes, wherein the therapeutic composition comprises at least one of pharmacologic agents, biologic agents, radiative agents, and combinations thereof.
In Example 11, the subject matter of Example undefined optionally includes, wherein at least a portion of the outer wall adjacent the second sub-chamber is permeable to permit elution of the therapeutic composition from the marker.
In Example 12, the subject matter of Example undefined optionally includes, wherein the secondary component comprises at least one solid identifying component configured to provide an identifying signal when an external imaging modality is applied.
In Example 13, the subject matter of Example undefined optionally includes, wherein the outer wall comprises a solid material including at least one of a glass material, a ceramic material, a polymer material or a composite material.
In Example 14, the subject matter of Example undefined optionally includes, wherein at least one of the sensing medium and the secondary component contains a contrast agent.
Example 15 is a method of manufacturing a radiographic marker capable of being permanently implanted in a living human or animal subject, the method comprising: providing a fully implantable, biocompatible container formed from a non-biodegradable solid material, the fully implantable, biocompatible container defining an internal chamber divided into at least a first sub-chamber and a second sub-chamber by an internal wall; filling the first sub-chamber with the sensing medium for producing a change in signal intensity when exposed to an external imaging modality; placing a secondary component within the second sub-chamber; sealing the first and second sub-chambers.
In Example 16, the subject matter of Example 15 optionally includes wherein the sensing medium produces a signal detectable by an imaging modality comprising at least one of MRI, ultrasound, x-ray, nuclear machine, infrared, fluorescence, and combinations thereof.
In Example 17, the subject matter of any one or more of Examples 15-16 optionally include wherein the secondary component comprises at least one of a second sensing medium, a therapeutic composition, a sensor, an identifying component, and combinations thereof.
In Example 18, the subject matter of Example 17 optionally includes wherein at least a portion of the implantable, biocompatible container adjacent the second sub-chamber is permeable.
In Example 19, the subject matter of any one or more of Examples 15-18 optionally include removably connecting a lid portion to the outer wall for accessing at least one of the first sub-chamber and the second sub-chamber.
In Example 20, the subject matter of Example 19 optionally includes wherein the outer wall further comprises: Removably connecting a second lid portion to the outer wall for accessing the other of the first sub-chamber and the second sub-chamber.
Each of these non-limiting examples can stand on its own, or can be combined in any permutation or combination with any one or more of the other examples.
The above detailed description includes references to the accompanying drawings, which form a part of the detailed description. The drawings show, by way of illustration, specific embodiments in which the present subject matter can be practiced. These embodiments are also referred to herein as “examples.” Such examples can include elements in addition to those shown or described. However, the present inventors also contemplate examples in which only those elements shown or described are provided. Moreover, the present inventors also contemplate examples using any combination or permutation of those elements shown or described (or one or more aspects thereof), either with respect to a particular example (or one or more aspects thereof), or with respect to other examples (or one or more aspects thereof) shown or described herein.
In the event of inconsistent usages between this document and any documents so incorporated by reference, the usage in this document controls.
In this document, the terms “a” or “an” are used, as is common in patent documents, to include one or more than one, independent of any other instances or usages of “at least one” or “one or more.” In this document, the term “or” is used to refer to a nonexclusive or, such that “A or B” includes “A but not B,” “B but not A,” and “A and B,” unless otherwise indicated. In this document, the terms “including” and “in which” are used as the plain-English equivalents of the respective terms “comprising” and “wherein,” Also, in the following claims, the terms “including” and “comprising” are open-ended, that is, a system, device, article, composition, formulation, or process that includes elements in addition to those listed after such a term in a claim are still deemed to fall within the scope of that claim. Moreover, in the following claims, the terms “first,” “second,” and “third,” etc. are used merely as labels, and are not intended to impose numerical requirements on their objects.
Method examples described herein can be machine or computer-implemented at least in part. Some examples can include a computer-readable medium or machine-readable medium encoded with instructions operable to configure an electronic device to perform methods as described in the above examples. An implementation of such methods can include code, such as microcode, assembly language code, a higher-level language code, or the like. Such code can include computer readable instructions for performing various methods. The code may form portions of computer program products. Further, in an example, the code can be tangibly stored on one or more volatile, non-transitory, or non-volatile tangible computer-readable media, such as during execution or at other times. Examples of these tangible computer-readable media can include, but are not limited to, hard disks, removable magnetic disks, removable optical disks (e.g., compact disks and digital video disks), magnetic cassettes, memory cards or sticks, random access memories (RAMs), read only memories (ROMs), and the like.
The above description is intended to be illustrative, and not restrictive. For example, the above-described examples (or one or more aspects thereof) may be used in combination with each other. Other embodiments can be used, such as by one of ordinary skill in the art upon reviewing the above description. The Abstract is provided to comply with 37 CFR. § 1.72(b), to allow the reader to quickly ascertain the nature of the technical disclosure. It is submitted with the understanding that it will not be used to interpret or limit the scope or meaning of the claims. Also, in the above Detailed Description, various features may be grouped together to streamline the disclosure. This should not be interpreted as intending that an unclaimed disclosed feature is essential to any claim. Rather, inventive subject matter may lie in less than all features of a particular disclosed embodiment. Thus, the following claims are hereby incorporated into the Detailed Description as examples or embodiments, with each claim standing on its own as a separate embodiment, and it is contemplated that such embodiments can be combined with each other in various combinations or permutations. The scope of the present subject matter should be determined with reference to the appended claims, along with the full scope of equivalents to which such claims are entitled.
This application is a continuation-in-part of U.S. patent application Ser. No. 14/966,400, filed Dec. 11, 2015, which is a continuation of U.S. patent application Ser. No. 14/634,965, filed Mar. 2, 2015, which is a continuation of Ser. No. 14/022,539, filed on Sep. 10, 2013, which is a continuation of U.S. Ser. No. 12/762,837, filed on Apr. 19, 2010, which is a continuation-in-Part of U.S. application Ser. No. 11/281,801, filed Nov. 17, 2005, and issued as U.S. Pat. No. 7,702,378 on Apr. 20, 2010, all of which are incorporated herein by reference in their entireties and the benefit of priority of each of which is claimed herein.
| Number | Name | Date | Kind |
|---|---|---|---|
| 2678195 | George | May 1954 | A |
| 5016639 | Allen | May 1991 | A |
| 5097839 | Allen | Mar 1992 | A |
| 5119817 | Allen | Jun 1992 | A |
| 5179955 | Leveen et al. | Jan 1993 | A |
| 5211164 | Allen | May 1993 | A |
| 5394457 | Leibinger | Feb 1995 | A |
| 5397329 | Allen | Mar 1995 | A |
| 5405402 | Dye et al. | Apr 1995 | A |
| 5469847 | Zinreich et al. | Nov 1995 | A |
| 5609850 | Deutsch et al. | Mar 1997 | A |
| 5702128 | Maxim et al. | Dec 1997 | A |
| 5769861 | Vilsmeier | Jun 1998 | A |
| 5782764 | Werne | Jul 1998 | A |
| 6128522 | Acker et al. | Oct 2000 | A |
| 6161034 | Burbank et al. | Dec 2000 | A |
| 6181960 | Jensen et al. | Jan 2001 | B1 |
| 6269148 | Jessop et al. | Jul 2001 | B1 |
| 6270464 | Fulton, III et al. | Aug 2001 | B1 |
| 6333971 | McCrory et al. | Dec 2001 | B2 |
| 6347241 | Burbank et al. | Feb 2002 | B2 |
| 6350244 | Fisher | Feb 2002 | B1 |
| 6356782 | Sirimanne et al. | Mar 2002 | B1 |
| 6371904 | Sirimanne et al. | Apr 2002 | B1 |
| 6374132 | Acker et al. | Apr 2002 | B1 |
| 6394965 | Klein | May 2002 | B1 |
| 6405072 | Cosman | Jun 2002 | B1 |
| 6419680 | Cosman | Jul 2002 | B1 |
| 6427081 | Burbank et al. | Jul 2002 | B1 |
| 6487438 | Widmark et al. | Nov 2002 | B1 |
| 6516211 | Acker et al. | Feb 2003 | B1 |
| 6544185 | Montegrande | Apr 2003 | B2 |
| 6546279 | Bova et al. | Apr 2003 | B1 |
| 6549802 | Thornton | Apr 2003 | B2 |
| 6567689 | Burbank et al. | May 2003 | B2 |
| 6575991 | Chesbrough et al. | Jun 2003 | B1 |
| 6605047 | Zarins et al. | Aug 2003 | B2 |
| 6632176 | McIntire et al. | Oct 2003 | B2 |
| 6635064 | U et al. | Oct 2003 | B2 |
| 6656192 | Espositio et al. | Dec 2003 | B2 |
| 6662041 | Burbank et al. | Dec 2003 | B2 |
| 6699205 | Fulton, III et al. | Mar 2004 | B2 |
| 6725083 | Burbank et al. | Apr 2004 | B1 |
| 6730042 | Fulton et al. | May 2004 | B2 |
| 6746661 | Kaplan | Jun 2004 | B2 |
| 6761679 | Sajo et al. | Jul 2004 | B2 |
| 6773408 | Acker et al. | Aug 2004 | B1 |
| 6778850 | Adler et al. | Aug 2004 | B1 |
| 6862470 | Burbank et al. | Mar 2005 | B2 |
| 6927406 | Zyromski | Aug 2005 | B2 |
| 6993375 | Burbank et al. | Jan 2006 | B2 |
| 6996433 | Burbank et al. | Feb 2006 | B2 |
| 7010340 | Scarantino et al. | Mar 2006 | B2 |
| 7044957 | Foerster et al. | May 2006 | B2 |
| 7047063 | Burbank et al. | May 2006 | B2 |
| 7226442 | Sheppard, Jr. et al. | Jun 2007 | B2 |
| 7668582 | Sirimanne et al. | Feb 2010 | B2 |
| 7702378 | Bolan et al. | Apr 2010 | B2 |
| 7792568 | Zhong et al. | Sep 2010 | B2 |
| 8280486 | Miller et al. | Oct 2012 | B2 |
| 8544162 | Bolan et al. | Oct 2013 | B2 |
| 8966735 | Bolan et al. | Mar 2015 | B2 |
| 9241773 | Bolan et al. | Jan 2016 | B2 |
| 9795455 | Bolan et al. | Oct 2017 | B2 |
| 9861450 | Bolan et al. | Jan 2018 | B2 |
| 20020035324 | Sirimanne et al. | Mar 2002 | A1 |
| 20020083591 | Geertsma et al. | Jul 2002 | A1 |
| 20020083951 | Stegmaier | Jul 2002 | A1 |
| 20020107437 | Sirimanne et al. | Aug 2002 | A1 |
| 20020161298 | Burbank et al. | Oct 2002 | A1 |
| 20020188196 | Burbank et al. | Dec 2002 | A1 |
| 20030023161 | Govari et al. | Jan 2003 | A1 |
| 20040030262 | Fisher | Feb 2004 | A1 |
| 20040176684 | Tabuchi | Sep 2004 | A1 |
| 20040186377 | Zhong | Sep 2004 | A1 |
| 20040193044 | Burbank et al. | Sep 2004 | A1 |
| 20040236211 | Burbank et al. | Nov 2004 | A1 |
| 20040236212 | Jones et al. | Nov 2004 | A1 |
| 20040236213 | Jones et al. | Nov 2004 | A1 |
| 20050004456 | Thomas et al. | Jan 2005 | A1 |
| 20050020916 | MacFarlane et al. | Jan 2005 | A1 |
| 20050033157 | Klein et al. | Feb 2005 | A1 |
| 20050035324 | McPeak et al. | Feb 2005 | A1 |
| 20050059884 | Kragg | Mar 2005 | A1 |
| 20050059888 | Sirimanne et al. | Mar 2005 | A1 |
| 20050065393 | Miller | Mar 2005 | A1 |
| 20050080337 | Sirimanne et al. | Apr 2005 | A1 |
| 20050080338 | Sirimanne et al. | Apr 2005 | A1 |
| 20050080339 | Sirimanne et al. | Apr 2005 | A1 |
| 20050085724 | Sirimanne et al. | Apr 2005 | A1 |
| 20050143656 | Burbank et al. | Jun 2005 | A1 |
| 20050154293 | Gisselberg | Jul 2005 | A1 |
| 20050205445 | Seiler et al. | Sep 2005 | A1 |
| 20050234336 | Beckman et al. | Oct 2005 | A1 |
| 20050255045 | Woltering | Nov 2005 | A1 |
| 20060036165 | Burbank et al. | Feb 2006 | A1 |
| 20060058645 | Komistek et al. | Mar 2006 | A1 |
| 20060058648 | Meier et al. | Mar 2006 | A1 |
| 20060079805 | Miller et al. | Apr 2006 | A1 |
| 20060084865 | Burbank et al. | Apr 2006 | A1 |
| 20060122503 | Burbank et al. | Jun 2006 | A1 |
| 20060155190 | Brubank et al. | Jul 2006 | A1 |
| 20060173296 | Miller et al. | Aug 2006 | A1 |
| 20060293581 | Plewes et al. | Dec 2006 | A1 |
| 20070087026 | Filed | Apr 2007 | A1 |
| 20070093726 | Leopold et al. | Apr 2007 | A1 |
| 20070110665 | Bolan et al. | May 2007 | A1 |
| 20070118034 | Mark | May 2007 | A1 |
| 20070142725 | Hardin et al. | Jul 2007 | A1 |
| 20070238984 | Maschke | Oct 2007 | A1 |
| 20080033286 | Whitmore et al. | Feb 2008 | A1 |
| 20080234572 | Jones | Sep 2008 | A1 |
| 20080269603 | Nicoson et al. | Oct 2008 | A1 |
| 20090069670 | Mark | Mar 2009 | A1 |
| 20090105584 | Jones | Apr 2009 | A1 |
| 20090213997 | Maschke | Aug 2009 | A1 |
| 20100030072 | Casanova | Feb 2010 | A1 |
| 20100121225 | Lewkowicz et al. | May 2010 | A1 |
| 20100287887 | Bolan et al. | Nov 2010 | A1 |
| 20110184279 | Massonneau | Jul 2011 | A1 |
| 20110276070 | Viray et al. | Nov 2011 | A1 |
| 20130046164 | Liu et al. | Feb 2013 | A1 |
| 20130150707 | Cima et al. | Jun 2013 | A1 |
| 20130324946 | Tobias et al. | Dec 2013 | A1 |
| 20140187911 | Bolan et al. | Jul 2014 | A1 |
| 20150173848 | Bolan et al. | Jun 2015 | A1 |
| 20160051337 | Bolan et al. | Feb 2016 | A1 |
| 20160010091 | Bolan et al. | Apr 2016 | A1 |
| Number | Date | Country |
|---|---|---|
| 2579914 | Nov 2006 | CA |
| 1802125 | Jul 2006 | CN |
| 102056544 | May 2011 | CN |
| 107205792 | Sep 2017 | CN |
| 107205792 | Jun 2020 | CN |
| 1491147 | Dec 2004 | EP |
| 1579878 | Sep 2005 | EP |
| 1847845 | Oct 2007 | EP |
| 3182919 | Oct 2018 | EP |
| 201143798 | Dec 2011 | TW |
| WO-9717103 | May 1997 | WO |
| WO-0024332 | May 2000 | WO |
| WO-0038579 | Jul 2000 | WO |
| WO-0230482 | Apr 2002 | WO |
| WO-03022133 | Mar 2003 | WO |
| WO-03051452 | Jun 2003 | WO |
| WO-2004084738 | Oct 2004 | WO |
| WO-2005046733 | May 2005 | WO |
| WO-2005063126 | Jul 2005 | WO |
| WO-06044132 | Apr 2006 | WO |
| WO-2006119645 | Nov 2006 | WO |
| WO-2007060576 | May 2007 | WO |
| 2012040455 | Mar 2012 | WO |
| WO-2016028976 | Feb 2016 | WO |
| WO-2016028976 | Feb 2016 | WO |
| Entry |
|---|
| “U.S. Appl. No. 11/281,801, Examiner Interview Summary dated Sep. 2, 2009”, 4 pgs. |
| “U.S. Appl. No. 11/281,801, Final Office Action dated Mar. 13, 2009”, 18 pgs. |
| “U.S. Appl. No. 11/281,801, Non-Final Office Action dated Sep. 22, 2008”, 12 pgs. |
| “U.S. Appl. No. 11/281,801, Notice of Allowance dated Dec. 2, 2009”, 10 pgs. |
| “U.S. Appl. No. 11/281,801, Response filed Dec. 18, 2008 to Non-Final Office Action dated Sep. 22, 2008”, 25 pgs. |
| “U.S. Appl. No. 11/281,801, Response filed Jun. 12, 2009 to Final Office Action dated Mar. 13, 2009”, 27 pgs. |
| “U.S. Appl. No. 11/281,801, Response filed Jul. 17, 2008 to Restriction Requirement dated Apr. 17, 2008”, 13 pgs. |
| “U.S. Appl. No. 11/281,801, Restriction Requirement dated Apr. 17, 2008”, 5 pgs. |
| “U.S. Appl. No. 11/281,801, Supplemental Response filed Aug. 24, 2009 to Final Office Action dated Mar. 13, 2009”, 29 pgs. |
| “U.S. Appl. No. 11/281,801, Supplemental Response filed Aug. 25, 2009 to Final Office Action dated Mar. 13, 2009”, 2 pgs. |
| “U.S. Appl. No. 11/281,801, Supplemental Response filed Aug. 28, 2009 to Final Office Action dated Mar. 13, 2009”, 16 pgs. |
| “U.S. Appl. No. 12/762,837, Non Final Office Action dated Nov. 2, 2012”, 15 pgs. |
| “U.S. Appl. No. 12/762,837, Notice of Allowance dated May 30, 2013”, 6 pgs. |
| “U.S. Appl. No. 12/762,837, Response filed Jan. 18, 2013 to Non Final Office Action dated Nov. 2, 2012”, 14 pgs. |
| “U.S. Appl. No. 14/022,539, Final Office Action dated Jul. 24, 2014”, 7 pgs. |
| “U.S. Appl. No. 14/022,539, Non Final Office Action dated Apr. 11, 2014”, 8 pgs. |
| “U.S. Appl. No. 14/022,539, Notice of Allowance dated Oct. 24, 2014”, 10 pgs. |
| “U.S. Appl. No. 14/022,539, Preliminary Amendment filed Mar. 10, 2014”, 8 pgs. |
| “U.S. Appl. No. 14/022,539, Response filed Jul. 11, 2014 to Non Final Office Action dated Apr. 11, 2014”, 10 pgs. |
| “U.S. Appl. No. 14/466,010, Advisory Action dated May 15, 2017”, 3 pgs. |
| “U.S. Appl. No. 14/466,010, Final Office Action dated Dec. 30, 2016”, 8 pgs. |
| “U.S. Appl. No. 14/466,010, Non Final Office Action dated Sep. 8, 2016”, 7 pgs. |
| “U.S. Appl. No. 14/466,010, Notice of Allowance dated Jun. 21, 2017”, 7 pgs. |
| “U.S. Appl. No. 14/466,010, Response filed May 1, 2017 to Final Office Action dated Dec. 30, 2016”, 12 pgs. |
| “U.S. Appl. No. 14/466,010, Response filed Dec. 1, 2016 to Non Final Office Action dated Sep. 8, 2016”, 12 pgs. |
| “U.S. Appl. No. 14/634,965, Non Final Office Action dated May 20, 2015”, 10 pgs. |
| “U.S. Appl. No. 14/634,965, Notice of Allowance dated Sep. 15, 2015”, 10 pgs. |
| “U.S. Appl. No. 14/634,965, Preliminary Amendment filed Mar. 3, 2015”, 9 pgs. |
| “U.S. Appl. No. 14/634,965, Response filed Apr. 28, 2015 to Restriction Requirement filed Apr. 8, 2015”, 9 pgs. |
| “U.S. Appl. No. 14/634,965, Response filed Aug. 18, 2015 to Non Final Office Action dated May 20, 2015”, 12 pgs. |
| “U.S. Appl. No. 14/634,965, Restriction Requirement dated Apr. 8, 2015”, 7 pgs. |
| “U.S. Appl. No. 14/966,400, Non Final Office Action dated May 2, 2017”, 10 pgs. |
| “U.S. Appl. No. 14/966,400, Notice of Allowance dated Aug. 30, 2017”, 5 pgs. |
| “U.S. Appl. No. 14/966,400, Preliminary Amendment filed Dec. 15, 2015”, 6 pgs. |
| “U.S. Appl. No. 14/966,400, Response filed Apr. 10, 2017 to Restriction Requirement dated Feb. 8, 2017”, 7 pgs. |
| “U.S. Appl. No. 14/966,400, Response filed Aug. 2, 2017 to Non Final Office Action dated May 2, 2017”, 9 pgs. |
| “U.S. Appl. No. 14/966,400, Restriction Requirement dated Feb. 8, 2017”, 7 pgs. |
| “International Application Serial No. PCT/US2015/046038, International Preliminary Report on Patentability dated Mar. 9, 2017”, 9 pgs. |
| “International Application Serial No. PCT/US2015/046038, International Search Report dated Oct. 21, 2015”, 4 pgs. |
| “International Application Serial No. PCT/US2015/046038, Written Opinion dated Oct. 21, 2015”, 7 pgs. |
| Bolan, P. J., et al., “A Novel Soft Tissue Marker for Multimodal Breast Imagine with Positive MRI Contrast”, Joint Annual Meeting ISMRM-ESMRMB, (May 2007), 1 pg. |
| Bolan, Patrick, “A Novel Tissue Marker for Multimodal Breast Imaging (Abstract)”, Abstract submitted Apr. 2005, published Radiological Society of North America (RSNA), Nov. 2005., [Online], Retrieved from the Internet: <URL: http://abstract.rsna.org/index.cfm?fuseaction˜submission.popupPrevie . . . >, (Nov. 2005), 2 pgs. |
| Bolan, Patrick, “Soft Tissue Markers or Clips (Presentation)”, This work was supported under NIH grants, the MIND institute, and the Keck Foundation., (Nov. 16, 2005), 16 pgs. |
| Ellis, R. E., et al., “Use of Biocompatible Fiducial Marker in Evaluating the Accuracy of CT Image Registration”, Investigative Radiology, (1996), 1-9. |
| Frank, Steven J., et al., “A Novel MRI Marker for Prostate Brachytherapy”, Int. J. Radiation Oncology Biol. Phys., vol. 70, No. 1, (2008), 5-8. |
| Gierga, D. P., et al., “The Correlation between Internal and External Markers for Abdominal Tumors: Implications for Respiratory Gating”, Int J Radial Oncol Biol Phys.; 61 (f); 1551-8, (Apr. 1, 2005), 1 pg. |
| Igdem, S., et al., “Implantation of Fiducial Markers for Image Guidance in Prostate Radiotherapy: Patient-reported toxicity”, The British Journal of Radiology, (2009), 1-5. |
| Maier-Hein, L, et al., “On Combining Internal and External Fiducials for Liver Motion Compensation”, Comput Aided Surg.; 13(6): 369-76, (Nov. 2008), 1 pg. |
| “European Application Serial No. 15756323.0, Response filed Oct. 6, 2017 to Communication pursuant to Rules 161(1) and 162 EPC dated Apr. 7, 2017”, 17 pgs. |
| “Chinese Application Serial No. 201580057297.8, Office Action dated Mar. 7, 2019”, w English Translation, 12 pgs. |
| “Chinese Application Serial No. 201580057297.8, Response filed Jan. 19, 2020 to Office Action dated Mar. 7, 2019”, with English claims, 11 pages. |
| “Canadian Application Serial No. 2,958,861, Voluntary Amendment filed Aug. 14, 2020”, 10 pages. |
| “Canadian Application Serial No. 2,958,861, Office Action dated Aug. 27, 2020”, 4 pages. |
| “Canadian Application Serial No. 2,958,861, Response filed Mar. 17, 2021 to Office Action dated Jan. 25, 2021”, 12 pgs. |
| “Canadian Application Serial No. 2,958,861, Office Action dated Jan. 25, 2021”, 4 pgs. |
| “Canadian Application Serial No. 2,958,861, Response filed Dec. 9, 2020 to Office Action dated Aug. 27, 2020”, 13 pgs. |
| “Canadian Application Serial No. 2,958,861, Office Action dated Jul. 22, 2021”, 4 pgs. |
| “Canadian Application Serial No. 2,958,861, Office Action dated Jul. 22, 2021”, 3 pgs. |
| U.S. Appl. No. 11/281,801 U.S. Pat. No. 7,702,378, filed Nov. 17, 2005, Tissue Marker for Multimodality Radiographic Imaging. |
| U.S. Appl. No. 12/762,837 U.S. Pat. No. 8,544,162, filed Apr. 19, 2010, Tissue Marker for Multimodality Radiographic Imaging. |
| U.S. Appl. No. 14/022,539 U.S. Pat. No. 8,966,735, filed Sep. 10, 2013, Tissue Marker for Multimodality Radiographic Imaging. |
| U.S. Appl. No. 14/634,965 U.S. Pat. No. 9,241,773, filed Mar. 2, 2015, Imaging Fiducial Markers and Methods. |
| U.S. Appl. No. 14/966,400, filed Dec. 11, 2015, Imaging Fiducial Markers and Methods. |
| U.S. Appl. No. 14/466,010 U.S. Pat. No. 9,795,455, filed Aug. 22, 2014, Tissue Marker for Multimodality Radiographic Imaging. |
| “Canadian Application Serial No. 2,958,861, Response filed Oct. 6, 2021 Office Action dated Jul. 22, 2021”, 18 pgs. |
| “Canadian Application 2,958,861 Commissioner's Notice—Application Found Allowable Nov. 17, 2017”, (Nov. 17, 2021), 1 page. |
| Number | Date | Country | |
|---|---|---|---|
| 20180085184 A1 | Mar 2018 | US |
| Number | Date | Country | |
|---|---|---|---|
| Parent | 14634965 | Mar 2015 | US |
| Child | 14966400 | US | |
| Parent | 14022539 | Sep 2013 | US |
| Child | 14634965 | US | |
| Parent | 12762837 | Apr 2010 | US |
| Child | 14022539 | US |
| Number | Date | Country | |
|---|---|---|---|
| Parent | 14966400 | Dec 2015 | US |
| Child | 15828021 | US | |
| Parent | 11281801 | Nov 2005 | US |
| Child | 12762837 | US |
