- Banga, Yasmin B;
- Lai, Yujung;
- Kim, Priscilla;
- Boeve, Bradley F;
- Boxer, Adam L;
- Rosen, Howard J;
- Forsberg, Leah K;
- Heuer, Hilary W;
- Brushaber, Danielle;
- Appleby, Brian;
- Biernacka, Joanna M;
- Bordelon, Yvette M;
- Botha, Hugo;
- Bozoki, Andrea C;
- Brannelly, Patrick;
- Dickerson, Brad C;
- Dickinson, Susan;
- Dickson, Dennis W;
- Domoto‐Reilly, Kimiko;
- Faber, Kelley;
- Fagan, Anne M;
- Fields, Julie A;
- Fishman, Ann;
- Foroud, Tatiana M;
- Galasko, Doug R;
- Gavrilova, Ralitza H;
- Gendron, Tania F;
- Geschwind, Daniel H;
- Ghoshal, Nupur;
- Goldman, Jill;
- Graff‐Radford, Jonathan;
- Graff‐Radford, Neill R;
- Grant, Ian;
- Grossman, Murray;
- Hsiung, Ging‐Yuek Robin;
- Huang, Eric J;
- Huey, Edward D;
- Irwin, David J;
- Jones, David T;
- Kantarci, Kejal;
- Karydas, Anna M;
- Kaufer, Daniel;
- Knopman, David S;
- Kramer, Joel H;
- Kremers, Walter K;
- Kornak, John;
- Kukull, Walter A;
- Lagone, Emma;
- Leger, Gabriel C;
- Litvan, Irene;
- Ljubenkov, Peter A;
- Lucente, Diane E;
- Mackenzie, Ian R;
- Manoochehri, Masood;
- Masdeu, Joseph C;
- McGinnis, Scott;
- Mendez, Mario F;
- Miller, Bruce L;
- Miyagawa, Toji;
- Nelson, Kevin M;
- Onyike, Chiadi U;
- Pantelyat, Alex;
- Pascual, Belen;
- Pearlman, Rodney;
- Petrucelli, Leonard;
- Pottier, Cyril P;
- Rademakers, Rosa;
- Ramos, Eliana Marisa;
- Rankin, Katherine P;
- Rascovsky, Katya;
- Rexach, Jessica E;
- Ritter, Aaron;
- Roberson, Erik D;
- Rojas, Julio C;
- Sabbagh, Marwan N;
- Salmon, David P;
- Savica, Rodolfo;
- Seeley, William W;
- Staffaroni, Adam M;
- Syrjanen, Jeremy A;
- Tartaglia, Maria Carmela;
- Tatton, Nadine;
- Taylor, Jack C;
- Toga, Arthur W;
- Weintraub, Sandra;
- Wheaton, Diana;
- Wong, Benjamin;
- Wszolek, Zbigniew;
- Consortium, ALLFTD
BACKGROUND: Frontotemporal lobar degeneration (FTLD) refers to a group of neurodegenerative conditions, affecting the frontal and/or temporal lobes. Ongoing research has provided insight into developing clinical trials for FTLD and key clinical measures such as structural MRI. To inform clinical trial design and optimize participation, it is imperative to explore facilitators and barriers for potential candidates. OBJECTIVE: The objective of this study is to explore facilitators and barriers to participating in future clinical trials for FTLD. METHODS: Advancing Research and Treatment for Frontotemporal Lobar Degeneration (ARTFL) and Longitudinal Evaluation of Familial Frontotemporal Dementia Subjects (LEFFTDS) are observational studies focused on characterizing FTLD syndromes in preparation for clinical trials. The 584 participants enrolled across 18 research sites in the United States and Canada completed a survey assessing interest in clinical trial participation. RESULTS: 29% of respondents self-reported as patients (63±10 years), 26% self-reported as caregivers answering on behalf of patients (65±10 years), and 45% self-reported as healthy but at risk for FTLD (48±14 years). Travel reimbursement was the most common factor reported to positively influence participation (≧66%), with the healthy but at risk group showing the strongest endorsement (83%). Cost and time involved in travel were possible barriers for about half of the patients (48%) and healthy but at risk respondents (53%). The respondents value receiving feedback on the study findings (≧80%) and being informed of their individual disease progression (≧75%). Particularly, keeping participation confidential was very important for the healthy but at risk group (62%). In regard to research assessments, most participants demonstrated a high interest in physical and neurological exams at a research center (≧87%) whereas only half were interested in doing more invasive procedures such as the lumbar puncture (≧52%). Overall, respondents showed a positive attitude and support for research participation (≧77%) and trusted that their health information would remain confidential in a clinical trial (≧53%). CONCLUSIONS: Favorable attitudes and interest towards medical research exist among participants. To optimize participation, clinical trials should allocate funding for travel and involve participants in feedback about study results and their disease progression. Alternatives to invasive assessments may increase participation.