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REALITY: Long-Term Real-World Outcomes Study on Patients Implanted With a Neurostimulator

Sponsor
Abbott Medical Devices (Industry)
Overall Status
Recruiting
CT.gov ID
NCT03876054
Collaborator
(none)
2,000
Enrollment
55
Locations
128.7
Anticipated Duration (Months)
36.4
Patients Per Site
0.3
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

The REALITY study is a prospective, post-market, non-randomized, multi-center, single-arm, open-label study intended to collect short- and long-term safety and effectiveness data on various populations implanted with Abbott's neurostimulation systems.

Condition or Disease Intervention/Treatment Phase
  • Device: Spinal cord stimulation (SCS)
  • Device: Dorsal root ganglion stimulation (DRG)

Detailed Description

This study has broad inclusion criteria and minimal exclusion criteria to ensure the results are representative of the real-world use of these devices. Enrollment caps will be implemented to ensure patients from approved indications are represented. Individuals who are scheduled to receive an implantable Abbott neurostimulation system are eligible for study consideration. The study will enroll up to 2,000 subjects from up to 100 participating centers. Subject enrollment is expected to be completed within 7 years; subjects will be followed for 5 years. The total duration of the study is expected to be 13 years, including enrollment, data collection from all subjects, and study close out.

Study Design

Study Type:
Observational
Anticipated Enrollment :
2000 participants
Observational Model:
Other
Time Perspective:
Prospective
Official Title:
Long-Term Real-World Outcomes Study on Patients Implanted With a Neurostimulator
Actual Study Start Date :
Mar 13, 2019
Anticipated Primary Completion Date :
Jun 1, 2029
Anticipated Study Completion Date :
Dec 1, 2029

Arms and Interventions

Arm Intervention/Treatment
Spinal cord stimulation (SCS)

Subjects using Abbott SCS systems

Device: Spinal cord stimulation (SCS)
Subjects will be implanted with market-released Abbott SCS systems
Dorsal root ganglion stimulation (DRG)

Subjects using Abbott DRG system

Device: Dorsal root ganglion stimulation (DRG)
Subjects will be implanted with market-released Abbott DRG system

Outcome Measures

Primary Outcome Measures

  1. Rate of device and procedure related adverse events, deaths, and device deficiencies [Baseline]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  2. Rate of device and procedure related adverse events, deaths, and device deficiencies [Permanent Implant Procedure]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  3. Rate of device and procedure related adverse events, deaths, and device deficiencies [6 months]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  4. Rate of device and procedure related adverse events, deaths, and device deficiencies [9 months]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be assessed via Telephone Calls and will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  5. Rate of device and procedure related adverse events, deaths, and device deficiencies [1 Year]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  6. Rate of device and procedure related adverse events, deaths, and device deficiencies [1.5 Years]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be assessed via Telephone Calls and will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  7. Rate of device and procedure related adverse events, deaths, and device deficiencies [2 Years]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  8. Rate of device and procedure related adverse events, deaths, and device deficiencies [2.5 Years]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be assessed via Telephone Calls and will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  9. Rate of device and procedure related adverse events, deaths, and device deficiencies [3 Years]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  10. Rate of device and procedure related adverse events, deaths, and device deficiencies [3.5 Years]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be assessed via Telephone Calls and will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  11. Rate of device and procedure related adverse events, deaths, and device deficiencies [4 Years]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  12. Rate of device and procedure related adverse events, deaths, and device deficiencies [4.5 Years]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be assessed via Telephone Calls and will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  13. Rate of device and procedure related adverse events, deaths, and device deficiencies [5 Years]

    Serious adverse device effects (SADEs), adverse device effects (ADEs), deaths, and device deficiencies will be summarized using counts, percentages or Kaplan-Meier survival estimates. This study has no primary or secondary endpoints, all endpoints are of equal weight.

Other Outcome Measures

  1. Mean Change in Clinical improvement from baseline to each follow up visit assessed by PROMIS-29 [6 months]

    The PROMIS-29 is used to estimate overall quality of life by assessing the following domains known to impact activities of daily living: physical function, sleep disturbance, depression, anxiety, fatigue, pain interference, pain intensity, and social role satisfaction. The scale requires subjects to rate the frequency and/or severity of symptoms and experiences related to each of these domains. The final item is an 11-point pain intensity numerical rating scale (NRS) by which the subject rates their average pain over the past 7 days. Subjects should read each item and check the one box that most closely represents their response. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  2. Mean Change in Clinical improvement from baseline to each follow up visit assessed by PROMIS-29 [1 Year]

    The PROMIS-29 is used to estimate overall quality of life by assessing the following domains known to impact activities of daily living: physical function, sleep disturbance, depression, anxiety, fatigue, pain interference, pain intensity, and social role satisfaction. The scale requires subjects to rate the frequency and/or severity of symptoms and experiences related to each of these domains. The final item is an 11-point pain intensity numerical rating scale (NRS) by which the subject rates their average pain over the past 7 days. Subjects should read each item and check the one box that most closely represents their response. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  3. Mean Change in Clinical improvement from baseline to each follow up visit assessed by PROMIS-29 [2 Years]

    The PROMIS-29 is used to estimate overall quality of life by assessing the following domains known to impact activities of daily living: physical function, sleep disturbance, depression, anxiety, fatigue, pain interference, pain intensity, and social role satisfaction. The scale requires subjects to rate the frequency and/or severity of symptoms and experiences related to each of these domains. The final item is an 11-point pain intensity numerical rating scale (NRS) by which the subject rates their average pain over the past 7 days. Subjects should read each item and check the one box that most closely represents their response. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  4. Mean Change in Clinical improvement from baseline to each follow up visit assessed by PROMIS-29 [3 Years]

    The PROMIS-29 is used to estimate overall quality of life by assessing the following domains known to impact activities of daily living: physical function, sleep disturbance, depression, anxiety, fatigue, pain interference, pain intensity, and social role satisfaction. The scale requires subjects to rate the frequency and/or severity of symptoms and experiences related to each of these domains. The final item is an 11-point pain intensity numerical rating scale (NRS) by which the subject rates their average pain over the past 7 days. Subjects should read each item and check the one box that most closely represents their response. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  5. Mean Change in Clinical improvement from baseline to each follow up visit assessed by PROMIS-29 [4 Years]

    The PROMIS-29 is used to estimate overall quality of life by assessing the following domains known to impact activities of daily living: physical function, sleep disturbance, depression, anxiety, fatigue, pain interference, pain intensity, and social role satisfaction. The scale requires subjects to rate the frequency and/or severity of symptoms and experiences related to each of these domains. The final item is an 11-point pain intensity numerical rating scale (NRS) by which the subject rates their average pain over the past 7 days. Subjects should read each item and check the one box that most closely represents their response. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  6. Mean Change in Clinical improvement from baseline to each follow up visit assessed by PROMIS-29 [5 Years]

    The PROMIS-29 is used to estimate overall quality of life by assessing the following domains known to impact activities of daily living: physical function, sleep disturbance, depression, anxiety, fatigue, pain interference, pain intensity, and social role satisfaction. The scale requires subjects to rate the frequency and/or severity of symptoms and experiences related to each of these domains. The final item is an 11-point pain intensity numerical rating scale (NRS) by which the subject rates their average pain over the past 7 days. Subjects should read each item and check the one box that most closely represents their response. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  7. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [6 months]

    The pain NRS consists of 1 question that will be asked by interviewing the subjects. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  8. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [9 months]

    The pain NRS consists of 1 question that will be asked to the subjects via telephone calls. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  9. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [1 year]

    The pain NRS consists of 1 question that will be asked by interviewing the subjects. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  10. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [1.5 years]

    The pain NRS consists of 1 question that will be asked to the subjects via telephone calls. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  11. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [2 Years]

    The pain NRS consists of 1 question that will be asked by interviewing the subjects. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  12. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [2.5 Years]

    The pain NRS consists of 1 question that will be asked to the subjects via telephone calls. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  13. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [3 Years]

    The pain NRS consists of 1 question that will be asked by interviewing the subjects. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  14. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [3.5 Years]

    The pain NRS consists of 1 question that will be asked to the subjects via telephone calls. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  15. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [4 Years]

    The pain NRS consists of 1 question that will be asked by interviewing the subjects. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  16. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [4.5 Years]

    The pain NRS consists of 1 question that will be asked to the subjects via telephone calls. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  17. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Numerical Rating Score (NRS) [5 Years]

    The pain NRS consists of 1 question that will be asked by interviewing the subjects. Patients will be asked to rate, from 0 (no pain) to 10 (worst imaginable pain), their pain at the time of study visit specific to the area(s) of chronic pain being treated. A higher score indicates greater pain intensity. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  18. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Catastrophizing Scale (PCS) [6 months]

    Pain Catastrophizing Scale is a validated scale that measures the magnitude of catastrophizing (negative thoughts and feelings while a patient is experiencing pain). Subjects answer questions about how they feel and what they think about when they are in pain (i.e., not at the current moment). The scale includes 13 statements concerning pain experiences that are rated on a scale between 0 'not at all' and 4 'all the time'. The scale is self-administered and takes 5 minutes to complete. A higher score indicates a higher level of catastrophizing. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  19. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Catastrophizing Scale (PCS) [1 Year]

    Pain Catastrophizing Scale is a validated scale that measures the magnitude of catastrophizing (negative thoughts and feelings while a patient is experiencing pain). Subjects answer questions about how they feel and what they think about when they are in pain (i.e., not at the current moment). The scale includes 13 statements concerning pain experiences that are rated on a scale between 0 'not at all' and 4 'all the time'. The scale is self-administered and takes 5 minutes to complete. A higher score indicates a higher level of catastrophizing. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  20. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Catastrophizing Scale (PCS) [2 Years]

    Pain Catastrophizing Scale is a validated scale that measures the magnitude of catastrophizing (negative thoughts and feelings while a patient is experiencing pain). Subjects answer questions about how they feel and what they think about when they are in pain (i.e., not at the current moment). The scale includes 13 statements concerning pain experiences that are rated on a scale between 0 'not at all' and 4 'all the time'. The scale is self-administered and takes 5 minutes to complete. A higher score indicates a higher level of catastrophizing. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  21. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Catastrophizing Scale (PCS) [3 Years]

    Pain Catastrophizing Scale is a validated scale that measures the magnitude of catastrophizing (negative thoughts and feelings while a patient is experiencing pain). Subjects answer questions about how they feel and what they think about when they are in pain (i.e., not at the current moment). The scale includes 13 statements concerning pain experiences that are rated on a scale between 0 'not at all' and 4 'all the time'. The scale is self-administered and takes 5 minutes to complete. A higher score indicates a higher level of catastrophizing. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  22. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Catastrophizing Scale (PCS) [4 Years]

    Pain Catastrophizing Scale is a validated scale that measures the magnitude of catastrophizing (negative thoughts and feelings while a patient is experiencing pain). Subjects answer questions about how they feel and what they think about when they are in pain (i.e., not at the current moment). The scale includes 13 statements concerning pain experiences that are rated on a scale between 0 'not at all' and 4 'all the time'. The scale is self-administered and takes 5 minutes to complete. A higher score indicates a higher level of catastrophizing. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  23. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Pain Catastrophizing Scale (PCS) [5 Years]

    Pain Catastrophizing Scale is a validated scale that measures the magnitude of catastrophizing (negative thoughts and feelings while a patient is experiencing pain). Subjects answer questions about how they feel and what they think about when they are in pain (i.e., not at the current moment). The scale includes 13 statements concerning pain experiences that are rated on a scale between 0 'not at all' and 4 'all the time'. The scale is self-administered and takes 5 minutes to complete. A higher score indicates a higher level of catastrophizing. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  24. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Oswestry Disability Index (ODI) [6 months]

    The ODI is a 10-item scale that evaluates disability related to low-back and leg pain. It is widely used, validated, and has been translated into several languages. Each section in the scale covers a different domain (pain intensity, personal care, lifting, walking, sitting, standing, sleeping, sex life, social life, and traveling). Each item is scored on a scale from 0-5 with the first item scored a "0" and representing no disability. The final item is scored a "5" and represents the maximum level of disability. If more than one response in a section is checked, the highest score is chosen. The scores for each section are summed for a final score ranging from 0 to 50. If an item is not answered, the total score is instead calculated as a percentage of the total possible score for all items that were completed. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  25. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Oswestry Disability Index (ODI) [1 Year]

    The ODI is a 10-item scale that evaluates disability related to low-back and leg pain. It is widely used, validated, and has been translated into several languages. Each section in the scale covers a different domain (pain intensity, personal care, lifting, walking, sitting, standing, sleeping, sex life, social life, and traveling). Each item is scored on a scale from 0-5 with the first item scored a "0" and representing no disability. The final item is scored a "5" and represents the maximum level of disability. If more than one response in a section is checked, the highest score is chosen. The scores for each section are summed for a final score ranging from 0 to 50. If an item is not answered, the total score is instead calculated as a percentage of the total possible score for all items that were completed. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  26. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Oswestry Disability Index (ODI) [2 Years]

    The ODI is a 10-item scale that evaluates disability related to low-back and leg pain. It is widely used, validated, and has been translated into several languages. Each section in the scale covers a different domain (pain intensity, personal care, lifting, walking, sitting, standing, sleeping, sex life, social life, and traveling). Each item is scored on a scale from 0-5 with the first item scored a "0" and representing no disability. The final item is scored a "5" and represents the maximum level of disability. If more than one response in a section is checked, the highest score is chosen. The scores for each section are summed for a final score ranging from 0 to 50. If an item is not answered, the total score is instead calculated as a percentage of the total possible score for all items that were completed. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  27. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Oswestry Disability Index (ODI) [3 Years]

    The ODI is a 10-item scale that evaluates disability related to low-back and leg pain. It is widely used, validated, and has been translated into several languages. Each section in the scale covers a different domain (pain intensity, personal care, lifting, walking, sitting, standing, sleeping, sex life, social life, and traveling). Each item is scored on a scale from 0-5 with the first item scored a "0" and representing no disability. The final item is scored a "5" and represents the maximum level of disability. If more than one response in a section is checked, the highest score is chosen. The scores for each section are summed for a final score ranging from 0 to 50. If an item is not answered, the total score is instead calculated as a percentage of the total possible score for all items that were completed. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  28. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Oswestry Disability Index (ODI) [4 Years]

    The ODI is a 10-item scale that evaluates disability related to low-back and leg pain. It is widely used, validated, and has been translated into several languages. Each section in the scale covers a different domain (pain intensity, personal care, lifting, walking, sitting, standing, sleeping, sex life, social life, and traveling). Each item is scored on a scale from 0-5 with the first item scored a "0" and representing no disability. The final item is scored a "5" and represents the maximum level of disability. If more than one response in a section is checked, the highest score is chosen. The scores for each section are summed for a final score ranging from 0 to 50. If an item is not answered, the total score is instead calculated as a percentage of the total possible score for all items that were completed. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  29. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Oswestry Disability Index (ODI) [5 Years]

    The ODI is a 10-item scale that evaluates disability related to low-back and leg pain. It is widely used, validated, and has been translated into several languages. Each section in the scale covers a different domain (pain intensity, personal care, lifting, walking, sitting, standing, sleeping, sex life, social life, and traveling). Each item is scored on a scale from 0-5 with the first item scored a "0" and representing no disability. The final item is scored a "5" and represents the maximum level of disability. If more than one response in a section is checked, the highest score is chosen. The scores for each section are summed for a final score ranging from 0 to 50. If an item is not answered, the total score is instead calculated as a percentage of the total possible score for all items that were completed. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  30. Mean Change in Clinical improvement from baseline to each follow up visit assessed by pain condition-related medication usage [6 months]

    Pain condition-related medication usage (e.g. opioids, anti-convulsants, anti-depressants, sleep aids, topicals) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  31. Mean Change in Clinical improvement from baseline to each follow up visit assessed by pain condition-related medication usage [1 Year]

    Pain condition-related medication usage (e.g. opioids, anti-convulsants, anti-depressants, sleep aids, topicals) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  32. Mean Change in Clinical improvement from baseline to each follow up visit assessed by pain condition-related medication usage [2 Years]

    Pain condition-related medication usage (e.g. opioids, anti-convulsants, anti-depressants, sleep aids, topicals) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  33. Mean Change in Clinical improvement from baseline to each follow up visit assessed by pain condition-related medication usage [3 Years]

    Pain condition-related medication usage (e.g. opioids, anti-convulsants, anti-depressants, sleep aids, topicals) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  34. Mean Change in Clinical improvement from baseline to each follow up visit assessed by pain condition-related medication usage [4 Years]

    Pain condition-related medication usage (e.g. opioids, anti-convulsants, anti-depressants, sleep aids, topicals) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  35. Mean Change in Clinical improvement from baseline to each follow up visit assessed by pain condition-related medication usage [5 Years]

    Pain condition-related medication usage (e.g. opioids, anti-convulsants, anti-depressants, sleep aids, topicals) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  36. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Transcutaneous Oxygen pressure measurement (TcPO2) [6 months]

    Transcutaneous Oxygen pressure measurement (TcPO2) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  37. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Transcutaneous Oxygen pressure measurement (TcPO2) [1 Year]

    Transcutaneous Oxygen pressure measurement (TcPO2) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  38. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Transcutaneous Oxygen pressure measurement (TcPO2) [2 Years]

    Transcutaneous Oxygen pressure measurement (TcPO2) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  39. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Transcutaneous Oxygen pressure measurement (TcPO2) [3 Years]

    Transcutaneous Oxygen pressure measurement (TcPO2) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  40. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Transcutaneous Oxygen pressure measurement (TcPO2) [4 Years]

    Transcutaneous Oxygen pressure measurement (TcPO2) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  41. Mean Change in Clinical improvement from baseline to each follow up visit assessed by Transcutaneous Oxygen pressure measurement (TcPO2) [5 Years]

    Transcutaneous Oxygen pressure measurement (TcPO2) will be summarized using mean, standard deviation, median, minimum, maximum, and a 95% confidence interval. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  42. Rate of patient satisfaction [6 months]

    Patient satisfaction will be summarized using counts and percentages This study has no primary or secondary endpoints, all endpoints are of equal weight.

  43. Rate of patient satisfaction [1 Year]

    Patient satisfaction will be summarized using counts and percentages This study has no primary or secondary endpoints, all endpoints are of equal weight.

  44. Rate of patient satisfaction [2 Years]

    Patient satisfaction will be summarized using counts and percentages This study has no primary or secondary endpoints, all endpoints are of equal weight.

  45. Rate of patient satisfaction [3 Years]

    Patient satisfaction will be summarized using counts and percentages This study has no primary or secondary endpoints, all endpoints are of equal weight.

  46. Rate of patient satisfaction [4 Years]

    Patient satisfaction will be summarized using counts and percentages This study has no primary or secondary endpoints, all endpoints are of equal weight.

  47. Rate of patient satisfaction [5 Years]

    Patient satisfaction will be summarized using counts and percentages This study has no primary or secondary endpoints, all endpoints are of equal weight.

  48. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [6 months]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via an interview technique. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better This study has no primary or secondary endpoints, all endpoints are of equal weight.

  49. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [9 months]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via telephone calls. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better This study has no primary or secondary endpoints, all endpoints are of equal weight.

  50. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [1 Year]

    The PGIC is a categorical rating scale used to evaluate the subject'simpression of change in his/her condition since the beginning of thestudy treatment. The subject will be requested to rate their overallchange in activity limitations, symptoms, emotions and overall qualityof life related to his/her condition on a seven-point categorical scale via an interview technique. The categories are as follows: 1-nochange, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  51. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [1.5 Year]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via telephone calls. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better This study has no primary or secondary endpoints, all endpoints are of equal weight.

  52. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [2 Years]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via an interview technique. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  53. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [2.5 Years]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via telephone calls. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better This study has no primary or secondary endpoints, all endpoints are of equal weight.

  54. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [3 Years]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via an interview technique. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  55. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [3.5 Years]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via telephone calls. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better This study has no primary or secondary endpoints, all endpoints are of equal weight.

  56. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [4 Years]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via an interview technique. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better. This study has no primary or secondary endpoints, all endpoints are of equal weight.

  57. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [4.5 Years]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via telephone calls. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better This study has no primary or secondary endpoints, all endpoints are of equal weight.

  58. Rate of Patient Global Impression of Change (PGIC) for global improvement of the patient. [5 Years]

    The PGIC is a categorical rating scale used to evaluate the subject's impression of change in his/her condition since the beginning of the study treatment. The subject will be requested to rate their overall change in activity limitations, symptoms, emotions and overall quality of life related to his/her condition on a seven-point categorical scale via an interview technique. The categories are as follows: 1-no change, 2-almost the same, 3-a little better, 4-somewhat better, 5-moderatly better, 6-better, and 7-a great deal better. This study has no primary or secondary endpoints, all endpoints are of equal weight.

Eligibility Criteria

Criteria

Ages Eligible for Study:
18 Years and Older
Sexes Eligible for Study:
All
Inclusion Criteria:

  1. Subject must provide written informed consent prior to any clinical investigation related procedure.

  2. Subject is at least 18 years (or the minimum age required by local law to consent for participation in a clinical investigation) or older at the time of enrollment.

  3. Subject is scheduled to have an Abbott neurostimulation system implanted within 60 days of baseline.

  4. Subject has a baseline (with no stimulation) pain NRS of ≥ 6.

Exclusion Criteria:

  1. Subject is enrolled, or intends to participate, in a competing clinical study, as determined by Abbott.

  2. Presence of other anatomic or comorbid conditions, or other medical, social, or psychological conditions that, in the investigator's opinion, could limit the subject's ability to participate in the clinical investigation or to comply with follow-up requirements.

  3. Subject has or is scheduled to receive an intrathecal pump.

  4. Subject is part of a vulnerable population.

  5. Subject has an existing implanted neuromodulation device to address their chronic pain.

Contacts and Locations

Locations

Site City State Country Postal Code
1 Phoenician Centers for Research & Innovation Phoenix Arizona United States 85021
2 Pain Institute of Southern Arizona Tucson Arizona United States 85718
3 California Orthopedics & Spine Larkspur California United States 94939
4 Restore Orthopedics & Spine Center Orange California United States 92868
5 Foothills Pain Management Clinic Pomona California United States 91767
6 Pacific Research Institute Santa Rosa California United States 95403
7 University of Florida Department of Anesthesia Gainesville Florida United States 32610
8 Rush University Medical Center Chicago Illinois United States 60612
9 University of Chicago Chicago Illinois United States 60637
10 Goodman Campbell Brain and Spine Indianapolis Indiana United States 46032
11 Nura Edina Minnesota United States 55435
12 Twin Cities Pain Clinic Edina Minnesota United States 55439
13 Mayo Clinic Rochester Minnesota United States 55905
14 Saint Louis Pain Consultants Chesterfield Missouri United States 63017
15 Advanced Pain Care Henderson Nevada United States 89052
16 Nevada Advanced Pain Specialists Reno Nevada United States 89511
17 Ainsworth Institute of Pain Management New York New York United States 10022
18 Unity Spine Center Rochester New York United States 14626
19 The Spine & Pain Institute of New York Staten Island New York United States 10305
20 Premier Pain Solutions Asheville North Carolina United States 28803
21 Adena Bone and Joint Center Chillicothe Ohio United States 45601
22 Premier Pain Treatment Institute Loveland Ohio United States 45140
23 Pacific Sports & Spine Eugene Oregon United States 97401
24 Spinal Diagnostics Tualatin Oregon United States 97062
25 Center for Interventional Pain & Spine Exton Pennsylvania United States 19341
26 Expert Pain Houston Texas United States 77079
27 Central Texas Pain Institute Killeen Texas United States 76542
28 Integrated Pain Associates Killeen Texas United States 76542
29 Advanced Pain Care Round Rock Texas United States 78664
30 The Spine & Nerve Center of St Francis Hospital Charleston West Virginia United States 25301
31 Metro Pain Group Clayton Victoria Australia 3168
32 Precision Brain, Spine & Pain Centre Kew Victoria Australia 3101
33 AZ Nikolaas Sint-Niklaas Eflndrs Belgium 9100
34 AZ Delta vzw Roeselare West Flanders Belgium 8800
35 Universitäts Klinikum Tübingen Tubingen Bad-wur Germany 72076
36 Klinikum Ingolstadt GmbH Ingolstadt Bavaria Germany 85049
37 Klinikum Duisburg GmbH Duisburg N. Rhin Germany 47055
38 Medizinische Einrichtungen der Universität Düsseldorf Dusseldorf N. Rhin Germany 40225
39 Krankenhaus Neuwerk Maria von den Aposteln Monchengladbach N. Rhin Germany 41066
40 Kliniken der Stadt Köln-Merheim Koln North Rhine-Westphalia Germany 51109
41 Universitätsklinikum Schleswig-Holstein Lübeck Schleswig-Holstein Germany 23538
42 Hospital Gera -Zentrum für interdisziplinäre Schmerztherapie Gera Thuringia Germany 07548
43 Krankenhaus Porz am Rhein Koln Germany 51149
44 Azienda Ospedaliera Monaldi Napoli Campani Italy 80131
45 Fondazione Salvatore Maugeri Pavia Lombard Italy 27100
46 Erasmus MC Rotterdam S Holln Netherlands 3015
47 St. Antonius Ziekenhuis Nieuwegein Utrecht Netherlands 3435 CM
48 Hospital Universitario de Salamanca Salamanca Cstleon Spain 37007
49 Hospital Universitario Puerta de Hierro Majadahonda Madrid Spain 28222
50 Hospital Universitari i Politècnic La Fe Valencia Spain 46026
51 Hôpital du Valais Sion Valais Switzerland 1951
52 Norfolk and Norwich Hospital Norwich England United Kingdom NR4 7UY
53 The Walton Centre Liverpool North West England United Kingdom L9 7LJ
54 Southmead Hospital Bristol Sowest United Kingdom BS10 5NB
55 Seacroft Hospital Leeds Yorkshire And The Humber United Kingdom LS14 6UH

Sponsors and Collaborators

  • Abbott Medical Devices

Investigators

  • Study Director: Ann Jannu, PhD, CCRP, Abbott

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.
Responsible Party:
Abbott Medical Devices
ClinicalTrials.gov Identifier:
NCT03876054
Other Study ID Numbers:
  • ABT-CIP-10279
First Posted:
Mar 15, 2019
Last Update Posted:
Feb 24, 2022
Last Verified:
Jan 1, 2022
Individual Participant Data (IPD) Sharing Statement:
No
Plan to Share IPD:
No
Studies a U.S. FDA-regulated Drug Product:
No
Studies a U.S. FDA-regulated Device Product:
Yes
Product Manufactured in and Exported from the U.S.:
No
Keywords provided by Abbott Medical Devices
spinal cord stimulation
dorsal root ganglion stimulation
Additional relevant MeSH terms:
Chronic Pain

Study Results

No Results Posted as of Feb 24, 2022