SPECIAL NOTICE
A -- Notice of Opportunity for Collaboration TYPE 1 DIABETES TRIALNET MULTI-CENTER CLINICAL TRIAL OF THE EFFECTS OF METABOLIC CONTROL ON PROGRESSION OF TYPE 1 DIABETES
- Notice Date
- 3/6/2007
- Notice Type
- Special Notice
- NAICS
- 541990
— All Other Professional, Scientific, and Technical Services
- Contracting Office
- Department of Health and Human Services, National Institutes of Health, Nat'l Institute of Diabetes, Digestive, & Kidney Diseases, 2 Democracy Plaza, Suite 700W 6707 Democracy Blvd., MSC 5455, Bethesda, MD, 20892-5455, UNITED STATES
- ZIP Code
- 00000
- Solicitation Number
- Reference-Number-DK-07-0079
- Response Due
- 4/30/2007
- Archive Date
- 5/15/2007
- Description
- Notice of Opportunity for Collaboration TYPE 1 DIABETES TRIALNET MULTI-CENTER CLINICAL TRIAL OF THE EFFECTS OF METABOLIC CONTROL ON PROGRESSION OF TYPE 1 DIABETES The National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) of the National Institutes of Health of the Public Health Service (PHS) of the Department of Health and Human Services (DHHS) seeks collaborations with Industry to provide insulin infusion pumps (CSIIs) and continuous blood glucose monitors for use in a NIH-sponsored multi-center trial to evaluate the effects of intensive metabolic control in newly-diagnosed type 1 diabetes using a glucose sensor-insulin infusion pump closed-loop system at the onset of diabetes followed by continuous real-time glucose monitoring associated with continuous insulin infusion therapy. INTRODUCTION: The National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) is planning to conduct a multi-center clinical trial to evaluate the safety and efficacy of tight metabolic control from diagnosis of type 1 diabetes on preservation of endogenous insulin production as measured by stimulated C-peptide. The trial will be conducted by investigators participating in the NIDDK sponsored TrialNet consortium. Study aims are to (1) determine if early and sustained restoration of metabolic control improves C-peptide production in patients with newly diagnosed type 1 diabetes compared to patients receiving routine diabetes management, and (2) to ascertain whether allowing surviving islet cells to be less metabolically active will impact the underlying autoimmune process of type 1 diabetes. The TrialNet Metabolic Control Study will enroll 108 patients, age 3-20 years, with newly diagnosed type 1 diabetes. Two-thirds of those enrolled will be randomized to the experimental treatment group while the other one-third will be randomized to standard treatment. Patients assigned to the experimental treatment group will have their insulin administered using a glucose sensor-insulin infusion pump closed-loop system within one week of diagnosis. If admitted for ketoacidosis, the closed-loop will begin when meals are initiated. The closed-loop system will consist of a subcutaneous glucose sensor with insulin pump for intravenous or subcutaneous insulin delivery. On discontinuing the closed-loop system, patients will be started on continuous subcutaneous glucose monitoring in real time in conjunction with an insulin infusion pump. Patients assigned to standard treatment will receive standard treatment for newly diagnosed type 1 diabetes. Study subjects will be enrolled over a one year period and then followed for two years. Primary outcome is the effect of tight metabolic control on the maintenance of the C-peptide area under the curve in response to a mixed meal at one year following enrollment and secondary outcomes will include the effect of metabolic control on immunologic assays relevant to type 1 diabetes. STUDY GOAL: The goal of this study is to determine whether intensive metabolic control of type 1 diabetes from the time of diagnosis preserves residual ?? cell function and therefore insulin secretion, improving blood glucose control and decreasing the negative short- and long-term consequences of hyperglycemia. CAPABILITY STATEMENT: The Collaborator Capability Statements?? received in response to this announcement will be reviewed by a Selection Committee. The Committee will utilize the information provided in the ??Collaborator Capability Statements?? received in response to this announcement to help in its deliberations. It is the intention of the NIDDK that all qualified Collaborators have the opportunity to provide information to the Selection Committee through their Capability Statements. The Capability Statement should not exceed ten (10) pages of narrative (not including appendices) and should address all of the following selection criteria: 1. Must provide evidence that the devices intended for use in the TrialNet metabolic control study have been issued a PMA, 510K or exemption registration number from the FDA. 2. Must provide most recently approved package inserts for such devices. 3. The statement should include a detailed plan demonstrating the ability to provide sufficient quantities of device(s) according to a mutually agreed upon schedule for the duration of the TrialNet metabolic control study to be conducted by TrialNet. 4. Must be prepared to supply their device(s) for immediate use in the TrialNet metabolic control study. 5. Must agree to have data collection and analysis performed by the TrialNet Coordinating Center (TNCC). 6. Provide the complete adverse event profile from human studies of the device(s). 7. Agree to share (with TrialNet) all unexpected serious adverse experience safety data from other studies involving their device(s). 8. Agree to have their device(s) used in conjunction with other device(s) used in the TrialNet metabolic control study. 9. Agree to having their device(s) used at all TrialNet study sites involved in the metabolic control study, including those in North America, Europe, Australia, and New Zealand. 10. The statement must address willingness to promptly publish research results. 11. Must include a description of the methods that would be used to assure privacy and maintain confidentiality of data. For the In-Hospital Closed Loop System: 1. The system should have a continuous glucose sensor (CGS) which communicates with either a computer or hand-held device (PDA). The computer or device must contain an algorithm for determining insulin delivery based on the CGS signal (absolute value and rate of change) and must then communicate the information to a subcutaneous insulin infusion pump. 2. The sensor should have accuracy with a MARD of <15% excluding glucose values used to calibrate the device. 3. The algorithm should have been previously tested in human subjects with at least 500 hours of viable clinical data. For the Out-Patient (Home) Real Time CGS Augmented Insulin Infusion Pump System: 1. The real-time CGS should provide data in real time with rate of change information and alarms for hyper- and hypoglycemia. 2. The insulin infusion pump should calculate insulin doses based on carbohydrate to insulin ratios and insulin sensitivity factors. 3. The information from the CGS and insulin infusion pump needs to be downloadable into an integrated database for the subject to review glucose trends and patterns in association with their insulin doses and carbohydrate intake. This data must be able to be viewed by subjects and study staff on a study website. 4. The information from the CGS and insulin infusion pump should be analyzable by a computer program which recognizes patterns and then provides study staff with recommendations for changes in insulin therapy which can then be communicated to the patient. 5. The Collaborator must be willing to work with the TrialNet Biostatistics Coordinating Center (BSC) to assure that the data generated by the CGS and insulin infusion pump is in a format compatible with the BSC database. Potential Industry Collaborators can provide some or all of the devices to be used during the TrialNet Metabolic Control study. Three to six TrialNet sites will conduct the study, and each site will need sufficient complete closed-loop apparatus for the study of two subjects simultaneously. In addition, the TrialNet sites will need to provide the components of the open-loop system to approximately 108 study subjects. Potential Collaborators should submit a brief capability statement to the contact person noted below. SUPPLEMENTARY INFORMATION: The Clinical Trial Agreement (CTA) into which the selected Collaborator is expected to enter is an agreement designed to enable a collaboration between Government laboratories and industry. IT IS NOT A GRANT, AND IS NOT A CONTRACT FOR THE PROCUREMENT OF GOODS OR SERVICES. The NIH is prohibited from transferring funds to a CTA collaborator. Under a CTA, NIH can contribute facilities, staff, materials, and expertise to the effort. The Collaborator typically contributes materials and expertise to the collaboration. This will be an in-kind collaborative arrangement. SUBMISSION DATES: Only written capability statements received by the NIDDK on or before April 30, 2007 will be considered. CONTACT INFORMATION: Capability Statements should be submitted to: Patricia M. Lake Deputy Director, Extramural Technology Transfer Office of Technology Transfer and Development National Institute of Diabetes and Digestive and Kidney Diseases, NIH 6707 Democracy Boulevard, Room 906B Bethesda, MD 20892 Phone: (301) 594-6762 Fax: (301) 480-7546 E-mail: lakep@mail.nih.gov For Scientific Inquiries contact: Ellen Leschek, M.D. Program Director, Type 1 Diabetes TrialNet Division of Diabetes, Endocrinology, and Metabolic Diseases National Institute of Diabetes and Digestive and Kidney Diseases, NIH 6707 Democracy Boulevard, Room 603 Bethesda, MD 20892 Phone: (301) 402-8291 Fax: (301) 480-3503 E-mail: LeschekE@extra.niddk.nih.gov A formatted version of the Notice of Opportunity will be posted at: http://TechDev.NIDDK.NIH.GOV/TrialNet.MetabolicControl
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