Search

Your search keyword '"Clarnette, R."' showing total 141 results
Start Over Author "Clarnette, R."
141 results on '"Clarnette, R."'

1. Dominantly Inherited Alzheimer Network Trials Unit (DIAN-TU): Trial Satisfaction and Attitudes towards Future Clinical Trials

Author

Liu, Haiyan, Li, J., Ziegemeier, E., Adams, S., McDade, E., Clifford, D. B., Cao, Y., Wang, G., Li, Y., Mills, S. L., Santacruz, A. M., Belyew, S., Grill, J. D., Snider, B. J., Mummery, C. J., Surti, G., Hannequin, D., Wallon, D., Berman, S. B., Jimenez-Velazquez, I. Z., Roberson, E. D., van Dyck, C. H., Honig, L. S., Sanchez-Valle, R., Brooks, W. S., Gauthier, S., Galasko, D., Masters, C. L., Brosch, J., Hsiung, G.-Y. R., Jayadev, S., Formaglio, M., Masellis, M., Clarnette, R., Pariente, J., Dubois, B., Pasquier, F., Bateman, R. J., and Llibre-Guerra, Jorge J.

Published
2024
Full Text
View/download PDF

2. The AUstralian multidomain Approach to Reduce dementia Risk by prOtecting brain health With lifestyle intervention study (AU-ARROW): A study protocol for a single-blind, multi-site, randomized controlled trial

Author

Gardener, SL, Fuller, SJ, Naismith, SL, Baker, L, Kivipelto, M, Villemagne, VL, Grieve, SM, Yates, P, Rainey-Smith, SR, Chen, J, Thompson, B, Armstrong, NJ, Fernando, MG, Blagojevic Castro, C, Meghwar, S, Raman, R, Gleason, A, Ireland, C, Clarnette, R, Anstey, KJ ; https://orcid.org/0000-0002-9706-9316, Taddei, K, Garg, M, Sohrabi, HR, Martins, RN, Gardener, SL, Fuller, SJ, Naismith, SL, Baker, L, Kivipelto, M, Villemagne, VL, Grieve, SM, Yates, P, Rainey-Smith, SR, Chen, J, Thompson, B, Armstrong, NJ, Fernando, MG, Blagojevic Castro, C, Meghwar, S, Raman, R, Gleason, A, Ireland, C, Clarnette, R, Anstey, KJ ; https://orcid.org/0000-0002-9706-9316, Taddei, K, Garg, M, Sohrabi, HR, and Martins, RN

Abstract

INTRODUCTION: The Finnish Geriatric Intervention Study (FINGER) led to the global dementia risk reduction initiative: World-Wide FINGERS (WW-FINGERS). As part of WW-FINGERS, the Australian AU-ARROW study mirrors aspects of FINGER, as well as US-POINTER. METHOD: AU-ARROW is a randomized, single-blind, multisite, 2-year clinical trial (n = 600; aged 55–79). The multimodal lifestyle intervention group will engage in aerobic exercise, resistance training and stretching, dietary advice to encourage MIND diet adherence, BrainHQ cognitive training, and medical monitoring and health education. The Health Education and Coaching group will receive occasional health education sessions. The primary outcome measure is the change in a global composite cognitive score. Extra value will emanate from blood biomarker analysis, positron emission tomography (PET) imaging, brain magnetic resonance imaging (MRI), and retinal biomarker tests. DISCUSSION: The finalized AU-ARROW protocol is expected to allow development of an evidence-based innovative treatment plan to reduce cognitive decline and dementia risk, and effective transfer of research outcomes into Australian health policy. Highlights: Study protocol for a single-blind, randomized controlled trial, the AU-ARROW Study. The AU-ARROW Study is a member of the World-Wide FINGERS (WW-FINGERS) initiative. AU-ARROW's primary outcome measure is change in a global composite cognitive score. Extra significance from amyloid PET imaging, brain MRI, and retinal biomarker tests. Leading to development of an innovative treatment plan to reduce cognitive decline.

Published
2024

3. Balance on the Brain: a randomised controlled trial evaluating the effect of a multimodal exercise programme on physical performance, falls, quality of life and cognition for people with mild cognitive impairment-study protocol

Author

Burton, E, Hill, K, Ellis, KA, Hill, A-M, Lowry, M, Moorin, R, McVeigh, JA, Jacques, A, Erickson, K, Tate, J, Bernard, S, Orr, CF, Bongiascia, L, Clarnette, R, Clark, ML, Williams, S, Lautenschlager, N, Burton, E, Hill, K, Ellis, KA, Hill, A-M, Lowry, M, Moorin, R, McVeigh, JA, Jacques, A, Erickson, K, Tate, J, Bernard, S, Orr, CF, Bongiascia, L, Clarnette, R, Clark, ML, Williams, S, and Lautenschlager, N

Abstract

INTRODUCTION: Exercise and physical activity have been shown to improve cognition for people living with mild cognitive impairment (MCI). There is strong evidence for the benefits of aerobic exercise and medium evidence for participating in regular strength training for people with MCI. However, people living with MCI fall two times as often as those without cognitive impairment and the evidence is currently unknown as to whether balance training for people with MCI is beneficial, as has been demonstrated for older people without cognitive impairment. The aim of this study is to determine whether a balance-focused multimodal exercise intervention improves balance and reduces falls for people with MCI, compared with a control group receiving usual care. METHODS AND ANALYSIS: This single blind randomised controlled trial (Balance on the Brain) will be offered to 396 people with MCI living in the community. The multimodal exercise intervention consists of two balance programmes and a walking programme to be delivered by physiotherapists over a 6-month intervention period. All participants will be followed up over 12 months (for the intervention group, this involves 6-month intervention and 6-month maintenance). The primary outcomes are (1) balance performance and (2) rate of falls. Physical performance, levels of physical activity and sedentary behaviour, quality of life and cognition are secondary outcomes. A health economic analysis will be undertaken to evaluate the cost-effectiveness of the intervention compared with usual care. ETHICS AND DISSEMINATION: Ethics approval has been received from the South Metropolitan Health Service Human Research Ethics Committee (HREC), Curtin University HREC and the Western Australia Department of Health HREC; and approval has been received to obtain data for health costings from Services Australia. The results will be disseminated through peer-review publications, conference presentations and online platforms. TRIAL REGISTRATION N

Published
2022

4. Early identification of frailty:Developing an international delphi consensus on pre-frailty

Author

Sezgin, D., O'Donovan, M., Woo, J., Bandeen-Roche, K., Liotta, G., Fairhall, N., Rodríguez-Laso, A., Apóstolo, J., Clarnette, R., Holland, C., Roller-Wirnsberger, R., Illario, M., Mañas, L.R., Vollenbroek-Hutten, M., Doğu, B.B., Balci, C., Pernas, F.O., Paul, C., Ahern, E., Romero-Ortuno, R., Molloy, W., Cooney, M.T., O'Shea, D., Cooke, J., Lang, D., Hendry, A., Kennelly, S., Rockwood, K., Clegg, A., Liew, A., O'Caoimh, R., Sezgin, D., O'Donovan, M., Woo, J., Bandeen-Roche, K., Liotta, G., Fairhall, N., Rodríguez-Laso, A., Apóstolo, J., Clarnette, R., Holland, C., Roller-Wirnsberger, R., Illario, M., Mañas, L.R., Vollenbroek-Hutten, M., Doğu, B.B., Balci, C., Pernas, F.O., Paul, C., Ahern, E., Romero-Ortuno, R., Molloy, W., Cooney, M.T., O'Shea, D., Cooke, J., Lang, D., Hendry, A., Kennelly, S., Rockwood, K., Clegg, A., Liew, A., and O'Caoimh, R.

Abstract

Background:: Frailty is associated with a prodromal stage called pre-frailty, a potentially reversible and highly prevalent intermediate state before frailty becomes established. Despite being widely-used in the literature and increasingly in clinical practice, it is poorly understood. Objective:: To establish consensus on the construct and approaches to diagnose and manage pre-frailty. Methods:: We conducted a modified (electronic, two-round) Delphi consensus study. The questionnaire included statements concerning the concept, aspects and causes, types, mechanism, assessment, consequences, prevention and management of pre-frailty. Qualitative and quantitative analysis methods were employed. An agreement level of 70% was applied. Results:: Twenty-three experts with different backgrounds from 12 countries participated. In total, 70 statements were circulated in Round 1. Of these, 52.8% were accepted. Following comments, 51 statements were re-circulated in Round 2 and 92.1% were accepted. It was agreed that physical and non-physical factors including psychological and social capacity are involved in the development of pre-frailty, potentially adversely affecting health and health-related quality of life. Experts considered pre-frailty to be an age-associated multi-factorial, multi-dimensional, and non-linear process that does not inevitably lead to frailty. It can be reversed or attenuated by targeted interventions. Brief, feasible, and validated tools and multidimensional assessment are recommended to identify pre-frailty. Conclusions:: Consensus suggests that pre-frailty lies along the frailty continuum. It is a multidimensional risk-state associated with one or more of physical impairment, cognitive decline, nutritional deficiencies and socioeconomic disadvantages, predisposing to the development of frailty. More research is needed to agree an operational definition and optimal management strategies.

Published
2022

5. Balance on the Brain: a randomised controlled trial evaluating the effect of a multimodal exercise programme on physical performance, falls, quality of life and cognition for people with mild cognitive impairment—study protocol

Author

Burton, E., Hill, K., Ellis, K.A., Hill, A-M, Lowry, M., Moorin, R., McVeigh, J.A., Jacques, A., Erickson, K.I., Tate, J., Bernard, S., Orr, C.F., Bongiascia, L., Clarnette, R., Clark, M.L., Williams, S., Lautenschlager, N., Burton, E., Hill, K., Ellis, K.A., Hill, A-M, Lowry, M., Moorin, R., McVeigh, J.A., Jacques, A., Erickson, K.I., Tate, J., Bernard, S., Orr, C.F., Bongiascia, L., Clarnette, R., Clark, M.L., Williams, S., and Lautenschlager, N.

Abstract

Introduction: Exercise and physical activity have been shown to improve cognition for people living with mild cognitive impairment (MCI). There is strong evidence for the benefits of aerobic exercise and medium evidence for participating in regular strength training for people with MCI. However, people living with MCI fall two times as often as those without cognitive impairment and the evidence is currently unknown as to whether balance training for people with MCI is beneficial, as has been demonstrated for older people without cognitive impairment. The aim of this study is to determine whether a balance-focused multimodal exercise intervention improves balance and reduces falls for people with MCI, compared with a control group receiving usual care. Methods and analysis: This single blind randomised controlled trial (Balance on the Brain) will be offered to 396 people with MCI living in the community. The multimodal exercise intervention consists of two balance programmes and a walking programme to be delivered by physiotherapists over a 6-month intervention period. All participants will be followed up over 12 months (for the intervention group, this involves 6-month intervention and 6-month maintenance). The primary outcomes are (1) balance performance and (2) rate of falls. Physical performance, levels of physical activity and sedentary behaviour, quality of life and cognition are secondary outcomes. A health economic analysis will be undertaken to evaluate the cost-effectiveness of the intervention compared with usual care. Ethics and dissemination: Ethics approval has been received from the South Metropolitan Health Service Human Research Ethics Committee (HREC), Curtin University HREC and the Western Australia Department of Health HREC; and approval has been received to obtain data for health costings from Services Australia. The results will be disseminated through peer-review publications, conference presentations and online platforms.

Published
2022

6. Early identification of frailty : Developing an international delphi consensus on pre-frailty

Author

Sezgin, D., O'Donovan, M., Woo, J., Bandeen-Roche, K., Liotta, G., Fairhall, N., Rodríguez-Laso, A., Apóstolo, J., Clarnette, R., Holland, C., Roller-Wirnsberger, R., Illario, M., Mañas, L.R., Vollenbroek-Hutten, M., Doğu, B.B., Balci, C., Pernas, F.O., Paul, C., Ahern, E., Romero-Ortuno, R., Molloy, W., Cooney, M.T., O'Shea, D., Cooke, J., Lang, D., Hendry, A., Kennelly, S., Rockwood, K., Clegg, A., Liew, A., O'Caoimh, R., Sezgin, D., O'Donovan, M., Woo, J., Bandeen-Roche, K., Liotta, G., Fairhall, N., Rodríguez-Laso, A., Apóstolo, J., Clarnette, R., Holland, C., Roller-Wirnsberger, R., Illario, M., Mañas, L.R., Vollenbroek-Hutten, M., Doğu, B.B., Balci, C., Pernas, F.O., Paul, C., Ahern, E., Romero-Ortuno, R., Molloy, W., Cooney, M.T., O'Shea, D., Cooke, J., Lang, D., Hendry, A., Kennelly, S., Rockwood, K., Clegg, A., Liew, A., and O'Caoimh, R.

Abstract

Background:: Frailty is associated with a prodromal stage called pre-frailty, a potentially reversible and highly prevalent intermediate state before frailty becomes established. Despite being widely-used in the literature and increasingly in clinical practice, it is poorly understood. Objective:: To establish consensus on the construct and approaches to diagnose and manage pre-frailty. Methods:: We conducted a modified (electronic, two-round) Delphi consensus study. The questionnaire included statements concerning the concept, aspects and causes, types, mechanism, assessment, consequences, prevention and management of pre-frailty. Qualitative and quantitative analysis methods were employed. An agreement level of 70% was applied. Results:: Twenty-three experts with different backgrounds from 12 countries participated. In total, 70 statements were circulated in Round 1. Of these, 52.8% were accepted. Following comments, 51 statements were re-circulated in Round 2 and 92.1% were accepted. It was agreed that physical and non-physical factors including psychological and social capacity are involved in the development of pre-frailty, potentially adversely affecting health and health-related quality of life. Experts considered pre-frailty to be an age-associated multi-factorial, multi-dimensional, and non-linear process that does not inevitably lead to frailty. It can be reversed or attenuated by targeted interventions. Brief, feasible, and validated tools and multidimensional assessment are recommended to identify pre-frailty. Conclusions:: Consensus suggests that pre-frailty lies along the frailty continuum. It is a multidimensional risk-state associated with one or more of physical impairment, cognitive decline, nutritional deficiencies and socioeconomic disadvantages, predisposing to the development of frailty. More research is needed to agree an operational definition and optimal management strategies.

Published
2022

11. AU‐ARROW (Australia)

Author

Martins, R.N., Anstey, K.J., Baker, L.D., Barin, E., Dias, C.B., Brown, B.M., Burnham, S.C., Chatterjee, P., Chen, J., Clarnette, R., Deang, K., England, T., Fuller, S., Gardener, S.L., Gleason, A., Grieve, S., Hillebrandt, H., Ireland, C., Kenny, P., Kivipelto, M., Mobbs, R., Naismith, S.L., Peters, Ruth, Rainey‐Smith, S.R., Raman, R., Savage, G., Sohrabi, H., Shah, T.M., Steiner, G.Z., Taddei, K., Thompson, B., Villemagne, V.L.L., Yates, P.A., Martins, R.N., Anstey, K.J., Baker, L.D., Barin, E., Dias, C.B., Brown, B.M., Burnham, S.C., Chatterjee, P., Chen, J., Clarnette, R., Deang, K., England, T., Fuller, S., Gardener, S.L., Gleason, A., Grieve, S., Hillebrandt, H., Ireland, C., Kenny, P., Kivipelto, M., Mobbs, R., Naismith, S.L., Peters, Ruth, Rainey‐Smith, S.R., Raman, R., Savage, G., Sohrabi, H., Shah, T.M., Steiner, G.Z., Taddei, K., Thompson, B., Villemagne, V.L.L., and Yates, P.A.

Abstract

Background The highly encouraging findings from the Finnish Geriatric Intervention Study (known as FINGER) led to the global initiative for dementia risk reduction known as world-wide FINGERS (WW FINGERS). As part of the collaboration, our Australian AU-ARROW trial will follow the general protocol of the FINGER trial, and will also be aligned with the U.S. arm of the study, US-POINTER, though will have minor cultural and dietary modifications to determine the validity of the intervention in an Australian setting. Method AU-ARROW is a randomised, single-blind 2-year clinical trial that will recruit 600 participants aged 60-79 satisfying specific inclusion/exclusion criteria, including normal cognition and one or more cardiovascular risk factors that place them at greater risk of cognitive decline. Participants will be distributed across two sites (a) Macquarie University Health Clinics, Sydney, NSW and (b) Sarich Neuroscience Research Institute, Edith Cowan University, Perth, WA, and will be randomised equally into either the innovative multi-modal intervention group or the study control group, who will receive general lifestyle advice and annual health check-ups, without treatment. Multi-modal intervention consists of aerobic exercise, resistance training and stretching; dietary advice with monitoring to encourage adherence to the MIND diet; cognitive training sessions via the Brain HQ computerised online training system; and medical monitoring and regular health education sessions. Heart rate trackers, diet and exercise log books, and the monitoring of Brain HQ sessions will all help with adherence. Primary outcome measure is improvement in global cognitive score, measured using neurocognitive tests identical to those in the US-POINTER protocol. Additional neurocognitive tests, physical function improvements, detailed diet monitoring and sleep monitoring will provide added data. The unique extra value of AU-ARROW trial consists of the testing for Alzheimer’s diseas

Published
2020

15. Rates of age‐ and amyloid β‐associated cortical atrophy in older adults with superior memory performance

Author

Dang, C., Yassi, N., Harrington, K.D., Xia, Y., Lim, Y.Y., Ames, D., Laws, S.M., Hickey, M., Rainey‐Smith, S., Sohrabi, H.R., Doecke, J.D., Fripp, J., Salvado, O., Snyder, P.J., Weinborn, M., Villemagne, V.L., Rowe, C.C., Masters, C.L., Maruff, P., Chambers, B., Chiu, E., Clarnette, R., Darby, D., Davison, M., Drago, J., Drysdale, P., Gilbert, J., Lim, K., Lautenschlager, N., LoGiudice, D., McCardle, P., McFarlane, S., Mander, A., Merory, J., O'Connor, D., Scholes, R., Samuel, M., Trivedi, D., Woodward, M., Dang, C., Yassi, N., Harrington, K.D., Xia, Y., Lim, Y.Y., Ames, D., Laws, S.M., Hickey, M., Rainey‐Smith, S., Sohrabi, H.R., Doecke, J.D., Fripp, J., Salvado, O., Snyder, P.J., Weinborn, M., Villemagne, V.L., Rowe, C.C., Masters, C.L., Maruff, P., Chambers, B., Chiu, E., Clarnette, R., Darby, D., Davison, M., Drago, J., Drysdale, P., Gilbert, J., Lim, K., Lautenschlager, N., LoGiudice, D., McCardle, P., McFarlane, S., Mander, A., Merory, J., O'Connor, D., Scholes, R., Samuel, M., Trivedi, D., and Woodward, M.

Abstract

Introduction Superior cognitive performance in older adults may reflect underlying resistance to age‐associated neurodegeneration. While elevated amyloid β (Aβ) deposition (Aβ+) has been associated with increased cortical atrophy, it remains unknown whether “SuperAgers” may be protected from Aβ‐associated neurodegeneration. Methods Neuropsychologically defined SuperAgers (n = 172) and cognitively normal for age (n = 172) older adults from the Australian Imaging, Biomarkers and Lifestyle study were case matched. Rates of cortical atrophy over 8 years were examined by SuperAger classification and Aβ status. Results Of the case‐matched SuperAgers and cognitively normal for age older adults, 40.7% and 40.1%, respectively, were Aβ+. Rates of age‐ and Aβ‐associated atrophy did not differ between the groups on any measure. Aβ− individuals displayed the slowest rates of atrophy. Discussion Maintenance of superior memory in late life does not reflect resistance to age‐ or Aβ‐associated atrophy. However, those individuals who reached old age without cognitive impairment nor elevated Aβ deposition (i.e. Aβ−) displayed reduced rates of cortical atrophy.

Published
2019

16. Comparison of Pittsburgh compound B and florbetapir in cross-sectional and longitudinal studies

Author

Su, Y, Flores, S, Wang, G, Hornbeck, RC, Speidel, B, Joseph-Mathurin, N, Vlassenko, AG, Gordon, BA, Koeppe, RA, Klunk, WE, Jack, CR, Farlow, MR, Salloway, S, Snider, BJ, Berman, SB, Roberson, ED, Brosch, J, Jimenez-Velazques, I, van Dyck, CH, Galasko, D, Yuan, SH, Jayadev, S, Honig, LS, Gauthier, S, Hsiung, GYR, Masellis, M, Brooks, WS ; https://orcid.org/0000-0001-8603-4233, Fulham, M, Clarnette, R, Masters, CL, Wallon, D, Hannequin, D, Dubois, B, Pariente, J, Sanchez-Valle, R, Mummery, C, Ringman, JM, Bottlaender, M, Klein, G, Milosavljevic-Ristic, S, McDade, E, Xiong, C, Morris, JC, Bateman, RJ, Benzinger, TLS, Su, Y, Flores, S, Wang, G, Hornbeck, RC, Speidel, B, Joseph-Mathurin, N, Vlassenko, AG, Gordon, BA, Koeppe, RA, Klunk, WE, Jack, CR, Farlow, MR, Salloway, S, Snider, BJ, Berman, SB, Roberson, ED, Brosch, J, Jimenez-Velazques, I, van Dyck, CH, Galasko, D, Yuan, SH, Jayadev, S, Honig, LS, Gauthier, S, Hsiung, GYR, Masellis, M, Brooks, WS ; https://orcid.org/0000-0001-8603-4233, Fulham, M, Clarnette, R, Masters, CL, Wallon, D, Hannequin, D, Dubois, B, Pariente, J, Sanchez-Valle, R, Mummery, C, Ringman, JM, Bottlaender, M, Klein, G, Milosavljevic-Ristic, S, McDade, E, Xiong, C, Morris, JC, Bateman, RJ, and Benzinger, TLS

Abstract

Introduction: Quantitative in vivo measurement of brain amyloid burden is important for both research and clinical purposes. However, the existence of multiple imaging tracers presents challenges to the interpretation of such measurements. This study presents a direct comparison of Pittsburgh compound B–based and florbetapir-based amyloid imaging in the same participants from two independent cohorts using a crossover design. Methods: Pittsburgh compound B and florbetapir amyloid PET imaging data from three different cohorts were analyzed using previously established pipelines to obtain global amyloid burden measurements. These measurements were converted to the Centiloid scale to allow fair comparison between the two tracers. The mean and inter-individual variability of the two tracers were compared using multivariate linear models both cross-sectionally and longitudinally. Results: Global amyloid burden measured using the two tracers were strongly correlated in both cohorts. However, higher variability was observed when florbetapir was used as the imaging tracer. The variability may be partially caused by white matter signal as partial volume correction reduces the variability and improves the correlations between the two tracers. Amyloid burden measured using both tracers was found to be in association with clinical and psychometric measurements. Longitudinal comparison of the two tracers was also performed in similar but separate cohorts whose baseline amyloid load was considered elevated (i.e., amyloid positive). No significant difference was detected in the average annualized rate of change measurements made with these two tracers. Discussion: Although the amyloid burden measurements were quite similar using these two tracers as expected, difference was observable even after conversion into the Centiloid scale. Further investigation is warranted to identify optimal strategies to harmonize amyloid imaging data acquired using different tracers.

Published
2019

17. Habitual exercise levels are associated with cerebral amyloid load in presymptomatic autosomal dominant Alzheimer's disease

Author

Brown, B.M., Sohrabi, H.R., Taddei, K., Gardener, S.L., Rainey-Smith, S.R., Peiffer, J.J., Xiong, C., Fagan, A.M., Benzinger, T., Buckles, V., Erickson, K.I., Clarnette, R., Shah, T., Masters, C.L., Weiner, M., Cairns, N., Rossor, M., Graff-Radford, N.R., Salloway, S., Vöglein, J., Laske, C., Noble, J., Schofield, P.R., Bateman, R.J., Morris, J.C., Martins, R.N., Brown, B.M., Sohrabi, H.R., Taddei, K., Gardener, S.L., Rainey-Smith, S.R., Peiffer, J.J., Xiong, C., Fagan, A.M., Benzinger, T., Buckles, V., Erickson, K.I., Clarnette, R., Shah, T., Masters, C.L., Weiner, M., Cairns, N., Rossor, M., Graff-Radford, N.R., Salloway, S., Vöglein, J., Laske, C., Noble, J., Schofield, P.R., Bateman, R.J., Morris, J.C., and Martins, R.N.

Abstract

Introduction: The objective of this study was to evaluate the relationship between self-reported exercise levels and Alzheimer's disease (AD) biomarkers, in a cohort of autosomal dominant AD mutation carriers. Methods: In 139 presymptomatic mutation carriers from the Dominantly Inherited Alzheimer Network, the relationship between self-reported exercise levels and brain amyloid load, cerebrospinal fluid (CSF) Aβ42, and CSF tau levels was evaluated using linear regression. Results: No differences in brain amyloid load, CSF Aβ42, or CSF tau were observed between low and high exercise groups. Nevertheless, when examining only those already accumulating AD pathology (i.e., amyloid positive), low exercisers had higher mean levels of brain amyloid than high exercisers. Furthermore, the interaction between exercise and estimated years from expected symptom onset was a significant predictor of brain amyloid levels. Discussion: Our findings indicate a relationship exists between self-reported exercise levels and brain amyloid in autosomal dominant AD mutation carriers.

Published
2017

18. High content, multi-parameter analyses in buccal cells to identify Alzheimer's disease

Author

François, M., Fenech, M., Thomas, P., Hor, M., Rembach, A., Martins, R.N., Rainey-Smith, S.R., Masters, C.L., Ames, D., Rowe, C.C., Macaulay, S.L., Hill, A.F., Leifert, W.R., Appannah, A., Barnes, M., Barnham, K., Bedo, J., Bellingham, S., Bon, L., Bourgeat, P., Brown, B., Buckley, R., Burnham, S., Bush, A., Chandler, G., Chen, K., Clarnette, R., Collins, S., Cooke, I., Cowie, T., Cox, K., Cuningham, E., Cyarto, E., Dang, P.A.V., Darby, D., Desmond, P., Doecke, J., Dore, V., Downing, H., Dridan, B., Duesing, K., Fahey, M., Farrow, M., Faux, N., Fernandez, S., Fernando, B., Fowler, C., Fripp, J., Frost, S., Gardener, S., Gibson, S., Graham, P., Gupta, V., Hansen, D., Harrington, K., Hone, E., Horne, M., Huckstepp, B., Jones, A., Jones, G., Kamer, A., Kanagasingam, Y., Keam, L., Kowalczyk, A., Krivdic, B., Lam, C.P., Lamb, F., Lautenschlager, N., Laws, S., Lenzo, N., Leroux, H., Lftikhar, F., Li, Q-X, Lim, F., Lim, L., Lockett, L., Lucas, K., Mano, M., Marczak, C., Martins, G., Matsumoto, Y., Bird, S., McBride, S., McKay, R., Mulligan, R., Nash, T., Nigro, J., O'Keefe, G., Ong, K., Parker, B., Pedrini, S., Peiffer, J., Pejoska, S., Penny, L., Perez, K., Pertile, K., Phal, P., Porter, T., Raniga, P., Restrepo, C., Riley, M., Roberts, B., Robertson, J., Rodrigues, M., Rooney, A., Rumble, R., Ryan, T., Salvado, O., Samuel, M., Saunders, I., Savage, G., Silbert, B., Sohrabi, H.R., Syrette, J., Szoeke, C., Taddei, K., Taddei, T., Tan, S., Tegg, M., Trivedi, D., Trounson, B., Veljanovski, R., Verdile, G., Villemagne, V., Volitakis, I., Vockler, C., Vovos, M., Vrantsidis, F., Walker, S., Watt, A., Weinborn, M., Wilson, B., Woodward, M., Yastrubetskaya, O., Yates, P., Zhang, P., Chatterjee, P., Creegan, R., De Ruyck, K., Ding, H., Groth, D., Head, R., Krause, D., Lachovitzki, R., Lim, Y.Y., Lintern, T., Mondal, A., Nuttall, S., O'Callaghan, N., Osborne, L., Pang, C., Patten, G., Tuckfield, A., Varghese, J., Wilson, A., Zhang, Q., François, M., Fenech, M., Thomas, P., Hor, M., Rembach, A., Martins, R.N., Rainey-Smith, S.R., Masters, C.L., Ames, D., Rowe, C.C., Macaulay, S.L., Hill, A.F., Leifert, W.R., Appannah, A., Barnes, M., Barnham, K., Bedo, J., Bellingham, S., Bon, L., Bourgeat, P., Brown, B., Buckley, R., Burnham, S., Bush, A., Chandler, G., Chen, K., Clarnette, R., Collins, S., Cooke, I., Cowie, T., Cox, K., Cuningham, E., Cyarto, E., Dang, P.A.V., Darby, D., Desmond, P., Doecke, J., Dore, V., Downing, H., Dridan, B., Duesing, K., Fahey, M., Farrow, M., Faux, N., Fernandez, S., Fernando, B., Fowler, C., Fripp, J., Frost, S., Gardener, S., Gibson, S., Graham, P., Gupta, V., Hansen, D., Harrington, K., Hone, E., Horne, M., Huckstepp, B., Jones, A., Jones, G., Kamer, A., Kanagasingam, Y., Keam, L., Kowalczyk, A., Krivdic, B., Lam, C.P., Lamb, F., Lautenschlager, N., Laws, S., Lenzo, N., Leroux, H., Lftikhar, F., Li, Q-X, Lim, F., Lim, L., Lockett, L., Lucas, K., Mano, M., Marczak, C., Martins, G., Matsumoto, Y., Bird, S., McBride, S., McKay, R., Mulligan, R., Nash, T., Nigro, J., O'Keefe, G., Ong, K., Parker, B., Pedrini, S., Peiffer, J., Pejoska, S., Penny, L., Perez, K., Pertile, K., Phal, P., Porter, T., Raniga, P., Restrepo, C., Riley, M., Roberts, B., Robertson, J., Rodrigues, M., Rooney, A., Rumble, R., Ryan, T., Salvado, O., Samuel, M., Saunders, I., Savage, G., Silbert, B., Sohrabi, H.R., Syrette, J., Szoeke, C., Taddei, K., Taddei, T., Tan, S., Tegg, M., Trivedi, D., Trounson, B., Veljanovski, R., Verdile, G., Villemagne, V., Volitakis, I., Vockler, C., Vovos, M., Vrantsidis, F., Walker, S., Watt, A., Weinborn, M., Wilson, B., Woodward, M., Yastrubetskaya, O., Yates, P., Zhang, P., Chatterjee, P., Creegan, R., De Ruyck, K., Ding, H., Groth, D., Head, R., Krause, D., Lachovitzki, R., Lim, Y.Y., Lintern, T., Mondal, A., Nuttall, S., O'Callaghan, N., Osborne, L., Pang, C., Patten, G., Tuckfield, A., Varghese, J., Wilson, A., and Zhang, Q.

Abstract

Alzheimer’s disease (AD) is a degenerative brain disorder and is the most common form of dementia. Minimally invasive approaches are required that combine biomarkers to identify individuals who are at risk of developing mild cognitive impairment (MCI) and AD, to appropriately target clinical trials for therapeutic discovery as well as lifestyle strategies aimed at prevention. Buccal mucosa cells from the Australian Imaging, Biomarkers and Lifestyle Flagship Study of Ageing cohort (n=60) were investigated for cytological markers that could be used to identify both MCI and AD individuals. Visual scoring of the buccal cytome demonstrated a significantly lower frequency of basal and karyorrhectic cells in the MCI group compared with controls. A high content, automated assay was developed using laser scanning cytometry to simultaneously measure cell types, nuclear DNA content and aneuploidy, neutral lipid content, putative Tau and amyloid-β (Aβ) in buccal cells. DNA content, aneuploidy, neutral lipids and Tau were similar in all groups. However, there was significantly lower Tau protein in both basal and karyolytic buccal cell types compared with differentiated buccal cells. Aβ, as measured by frequency of cells containing Aβ signal, as well as area and integral of Aβ signal, was significantly higher in the AD group compared with the control group. Buccal cell Aβ was correlated with mini-mental state examination (MMSE) scores (r = -0.436, P=0.001) and several blood-based biomarkers. Combining newly identified biomarkers from buccal cells with those already established may offer a potential route for more specific biomarker panels which may substantially increase the likelihood of better predictive markers for earlier diagnosis of AD.

Published
2016

19. MEASURING THE EFFECT OF CARERS ON PATIENTS’ RISK OF ADVERSE HEALTHCARE OUTCOMES USING THE CAREGIVER NETWORK SCORE

Author

O’CAOIMH, R., primary, CORNALLY, N., additional, SVENDROVSKI, A., additional, WEATHERS, E., additional, FITZGERALD, C., additional, HEALY, E., additional, O’CONNELL, E., additional, O’KEEFFE, G., additional, O’HERLIHY, E., additional, GAO, Y., additional, O’DONNELL, R., additional, O’SULLIVAN, R., additional, LEAHY-WARREN, P., additional, ORFILA, F., additional, PAÚL, C., additional, CLARNETTE, R., additional, and MOLLOY, D.W., additional

Published
2016
Full Text
View/download PDF

20. COLLaboration on AGEing-COLLAGE: Ireland's three star reference site for the European Innovation Partnership on Active and Healthy Ageing (EIP on AHA)

Author

O’Caoimh, R., primary, Sweeney, C., additional, Hynes, H., additional, McGlade, C., additional, Cornally, N., additional, Daly, E., additional, Weathers, E., additional, Coffey, A., additional, FitzGerald, C., additional, Healy, E., additional, O’Connell, E., additional, O’Keeffe, G., additional, O'Sullivan, R., additional, Timmons, S., additional, Foley, T., additional, Creed, E., additional, Hynes, M., additional, Twomey, A., additional, Sammon, M., additional, Cullen, D., additional, Mullan, E., additional, Orfila, F., additional, Paúl, C., additional, Clarnette, R., additional, Campbell, S., additional, Lupari, M., additional, McCarthy, S., additional, Sahm, L., additional, Byrne, S., additional, O’Leary, C., additional, O'Shea, S., additional, O’Donoghue, J., additional, McAdoo, J., additional, Kearney, P.M., additional, Galvin, P., additional, O’Byrne-Maguire, I., additional, Browne, J., additional, Kenny, R., additional, O’Herlihy, E., additional, O’Toole, P., additional, McFarlane, A., additional, Deery, M., additional, Bond, R., additional, Martin, J., additional, Shorten, G., additional, and Molloy, W., additional

Published
2015
Full Text
View/download PDF

21. Quantitative MR Imaging R(2) Relaxometry in Elderly Participants Reporting Memory Loss

Author

House, M.J., St. Pierre, T.G., Foster, J.K., Martins, R.N., and Clarnette, R.

Subjects
Aged, 80 and over, Male, Iron, Statistics as Topic, Brain, Middle Aged, Water-Electrolyte Balance, Magnetic Resonance Imaging, Alzheimer Disease, Neuropsychology, Reference Values, Image Processing, Computer-Assisted, Homeostasis, Humans, Female, Amnesia, Aged, Demyelinating Diseases
Abstract

BACKGROUND AND PURPOSE: In Alzheimer disease (AD), elevated brain iron concentrations in gray matter suggest a disruption in iron homeostasis, while demyelination processes in white matter increase the water content. Our aim was to assess whether the transverse proton relaxation rate, or R(2), an MR imaging parameter affected by changes in brain iron concentration and water content, was different in elderly participants with mild to severe levels of cognitive impairment compared with healthy controls. METHODS: Twelve elderly participants reporting memory problems and 11 healthy volunteers underwent single-spin-echo MR imaging in a 1.5T scanner, with subsequent neuropsychological testing. R(2) data were collected from 14 brain regions in cortical and subcortical gray and white matter. Those with memory complaints were separated into 2 further subgroups: MC1 (no objective cognitive impairment) and MC2 (mild to severe objective cognitive impairment). RESULTS: Mean brain R(2) values from the 11 controls correlated strongly (r = 0.94, P < .0001) with reference brain iron concentrations for healthy adults. R(2) values in the MC1 and MC2 subgroups were significantly higher in the right temporal cortex and significantly lower in the left internal capsule, compared with healthy controls. R(2) values in the MC2 subgroup were significantly lower in the left temporal and frontal white matter, compared with healthy controls. CONCLUSIONS: R(2) differences between both subgroups and the healthy controls suggest iron has increased in the temporal cortex, and myelin has been lost from several white matter regions in those with memory complaints, consistent with incipient AD pathogenesis and biochemical data.

Published
2006

22. COMPONENTS OF THE RISK INSTRUMENT FOR SCREENING IN THE COMMUNITY (RISC) THAT CORRELATE WITH PUBLIC HEALTH NURSES’ PERCEPTION OF RISK

Author

LEAHY-WARREN, P., primary, O’CAOIMH, R., additional, FITZGERALD, C., additional, COCHRANE, A., additional, SVENDROVSKI, A., additional, CRONIN, U., additional, O’HERLIHY, E., additional, CORNALLY, N., additional, GAO, Y., additional, HEALY, E., additional, O’CONNELL, E., additional, O’KEEFFE, G., additional, COVENEY, S., additional, MCGLYNN, J., additional, CLARNETTE, R., additional, and MOLLOY, D.W., additional

Published
2015
Full Text
View/download PDF

23. New lexicon and criteria for the diagnosis of Alzheimer's disease

Author

Sohrabi, H.R., Weinborn, M., Badcock, J., Bates, K.A., Clarnette, R., Trivedi, D., Verdile, G., Sutton, T., Lenzo, N.P., Gandy, S.E., Martins, R.N., Sohrabi, H.R., Weinborn, M., Badcock, J., Bates, K.A., Clarnette, R., Trivedi, D., Verdile, G., Sutton, T., Lenzo, N.P., Gandy, S.E., and Martins, R.N.

Abstract

We have been following the proposed diagnostic criteria for Alzheimer's disease (AD) closely over the past few years. 1 Recent revisions of the AD criteria proposed by Dubois and colleagues 2 represent a clear improvement on their previously published Position Paper. 3 In the new revision, Dubois and colleagues propose an important distinction between the clinical disorder (AD) and the neuropathological condition (“Alzheimer's pathology”). They also describe several distinctions within the clinical disorder, including two preclinical conditions (“asymptomatic at-risk for AD” and “presymptomatic AD”), a prodromal condition (“prodromal AD”), and AD dementia with varying presentations (“typical AD,” “atypical AD”, and “mixed AD”)...

Published
2011

25. Vitamins B12, B6, and folic acid for cognition in older men

Author

Ford, A., Flicker, L., Alfonso, Helman, Thomas, J., Clarnette, R., Martins, R., Almeida, O., Ford, A., Flicker, L., Alfonso, Helman, Thomas, J., Clarnette, R., Martins, R., and Almeida, O.

Abstract

Objective: To investigate whether supplementing older men with vitamins B12, B6, and folic acid improves cognitive function. Methods: The investigators recruited 299 community-representative hypertensive men 75 years and older to a randomized, double-blind controlled clinical trial of folic acid, vitamin B6, and B12 supplementation vs placebo over 2 years. The primary outcome of interest was the change in the cognitive subscale of the Alzheimer's Disease Assessment Scale (ADAS-cog). A secondary aim of the study was to determine if supplementation with vitamins decreased the risk of cognitive impairment and dementia over 8 years. Results: The groups were well-balanced for demographic and biochemical parameters. There was no difference in the ADAS-cog change from baseline to 24 months between the placebo (0.8, SD 4.0) and vitamins group (0.7, SD 3.4). The adjusted scores in the treatment groups did not differ over time (placebo 0.2 lower, z = 0.71, p = 0.478). There was a nonsignificant 28% decrease in the risk of cognitive impairment (odds ratio 0.72, 95% confidence interval 0.25-2.09) and dementia (hazard ratio 0.72, 95% confidence interval 0.29-1.78) over 8 years of follow-up. Conclusions: The daily supplementation of vitamins B12, B6, and folic acid does not benefit cognitive function in older men, nor does it reduce the risk of cognitive impairment or dementia. Classification of Evidence: This study provides Class I evidence that vitamin supplementation with daily doses of 400 µg of B12, 2 mg of folic acid, and 25 mg of B6 over 2 years does not improve cognitive function in hypertensive men aged 75 and older. Copyright © 2010 by AAN Enterprises, Inc.

Published
2010

27. The Australian Imaging, Biomarkers and Lifestyle (AIBL) study of aging: methodology and baseline characteristics of 1112 individuals recruited for a longitudinal study of Alzheimer’s disease

Author

Ellis, K., Bush, A., Darby, D., de Fazio, D., Foster, Jonathan, Hudson, P., Lautenschlager, N., Lenzo, N., Martins, R., Maruff, P., Masters, C., Milner, A., Pike, K., Rowe, C., Savage, G., Szoeke, C., Taddei, K., Villemagne, V., Woodward, M., Ames, D., Acosta, O., Ames, J., Agarwal, M., Bahar-Fuchs, A., Baxendale, D., Bechta-Metti, K., Bevage, C., Bevege, L., Bourgeat, P., Brown, B., Clarnette, R., Cowie, T., Crowley, K., Currie, A., El- Sheikh, D., Dickinson, K., Farrow, M., Faux, N., Fripp, J., Fowler, C., Gupta, V., Jones, G., Khoo, J., Killedar, A., Killeen, N., Kim, T.W., Kotsopoulos, E., Lachovitzki, R., Li, Q., Liang, X., Lucas, K., Lui, J., Martins, G., Montague, C., Moore, L., Muir, A., O’Halloran, C., O’Keefe, G., Panayiotou, A., Paton, A., Paton, J., Peiffer, J., Pejoska, S., Pertile, K., Porter, L., Price, R., Raniga, P., Rees, G., Rembach, A., Rimajova, M., Robins, P., Ronsisvalle, E., Rumble, R., Rodrigues, M., Salvado, O., Sach, J., Samuel, M., Sittironnarit, G., Taddei, T., Trivedi, D., Trounson, B., Tsikkos, M., Walker, S., Ward, V., Yastrubetskaya, O., Ellis, K., Bush, A., Darby, D., de Fazio, D., Foster, Jonathan, Hudson, P., Lautenschlager, N., Lenzo, N., Martins, R., Maruff, P., Masters, C., Milner, A., Pike, K., Rowe, C., Savage, G., Szoeke, C., Taddei, K., Villemagne, V., Woodward, M., Ames, D., Acosta, O., Ames, J., Agarwal, M., Bahar-Fuchs, A., Baxendale, D., Bechta-Metti, K., Bevage, C., Bevege, L., Bourgeat, P., Brown, B., Clarnette, R., Cowie, T., Crowley, K., Currie, A., El- Sheikh, D., Dickinson, K., Farrow, M., Faux, N., Fripp, J., Fowler, C., Gupta, V., Jones, G., Khoo, J., Killedar, A., Killeen, N., Kim, T.W., Kotsopoulos, E., Lachovitzki, R., Li, Q., Liang, X., Lucas, K., Lui, J., Martins, G., Montague, C., Moore, L., Muir, A., O’Halloran, C., O’Keefe, G., Panayiotou, A., Paton, A., Paton, J., Peiffer, J., Pejoska, S., Pertile, K., Porter, L., Price, R., Raniga, P., Rees, G., Rembach, A., Rimajova, M., Robins, P., Ronsisvalle, E., Rumble, R., Rodrigues, M., Salvado, O., Sach, J., Samuel, M., Sittironnarit, G., Taddei, T., Trivedi, D., Trounson, B., Tsikkos, M., Walker, S., Ward, V., and Yastrubetskaya, O.

Abstract

Background: The Australian Imaging, Biomarkers and Lifestyle (AIBL) flagship study of aging aimed to recruit 1000 individuals aged over 60 to assist with prospective research into Alzheimer's disease (AD). This paper describes the recruitment of the cohort and gives information about the study methodology, baseline demography, diagnoses, medical comorbidities, medication use, and cognitive function of the participants. Methods: Volunteers underwent a screening interview, had comprehensive cognitive testing, gave 80 ml of blood, and completed health and lifestyle questionnaires. One quarter of the sample also underwent amyloid PET brain imaging with Pittsburgh compound B (PiB PET) and MRI brain imaging, and a subgroup of 10% had ActiGraph activity monitoring and body composition scanning. Results: A total of 1166 volunteers were recruited, 54 of whom were excluded from further study due to comorbid disorders which could affect cognition or because of withdrawal of consent. Participants with AD (211) had neuropsychological profiles which were consistent with AD, and were more impaired than participants with mild cognitive impairment (133) or healthy controls (768), who performed within expected norms for age on neuropsychological testing. PiB PET scans were performed on 287 participants, 100 had DEXA scans and 91 participated in ActiGraph monitoring. Conclusion: The participants comprising the AIBL cohort represent a group of highly motivated and well-characterized individuals who represent a unique resource for the study of AD. They will be reassessed at 18-month intervals in order to determine the predictive utility of various biomarkers, cognitive parameters and lifestyle factors as indicators of AD, and as predictors of future cognitive decline.

Published
2009

30. ADVANCE CARE PLANNING, A STEP-BY-STEP GUIDE FOR HEALTH CARE PROFESSIONALS ASSISTING PATIENTS WITH CHRONIC CONDITIONS TO PLAN FOR CARE TOWARDS END OF LIFE

Author

Greeve, K, primary, Bloomer, S, additional, Chellew-Hawley, M, additional, Clarnette, R, additional, Fortnum, D, additional, Garton-Smith, J, additional, Harney, M, additional, Ibrahim, J, additional, Kendall, P, additional, Koay, A, additional, Moody, H, additional, Porter, S, additional, Scarff, Z, additional, Trevaskis, G, additional, Yuen, K, additional, and Walker, H, additional

Published
2013
Full Text
View/download PDF

31. Inspection time in non-demented older adults with mild cognitive impairment

Author

Bonney, K.R., Almeida, O.P., Flicker, L., Davies, S., Clarnette, R., Anderson, M., Lautenschlager, N.T., Bonney, K.R., Almeida, O.P., Flicker, L., Davies, S., Clarnette, R., Anderson, M., and Lautenschlager, N.T.

Abstract

The aim of this study was to examine inspection time (IT) performance in older adults with mild cognitive impairment (MCI), who are at higher risk of developing further cognitive decline or dementia. IT is described as an index of speed of informational intake. IT correlates with measures of fluid intelligence and is possibly a marker for the integrity of the cholinergic system of the brain. IT may therefore be useful in aiding the diagnosis of early-stage progressive cognitive impairment. The current study compares IT in 28 people with MCI to 28 age, gender and education-matched controls. The computer-based, visual IT task required participants to discriminate between two visual stimuli that were presented for brief periods. Participants' IT performance was compared to their performance on cognitive and memory tasks. Group comparison showed that participants with MCI performed significantly worse on IT than controls and was not affected by years of education. In combination with other clinical, neuropsychological and biological tests, IT may be a useful assessment tool for improving the identification of older adults at risk for clinically relevant cognitive decline.

Published
2006

32. Oestrogen replacement therapy may improve memory functioning in the absence of APOE e4

Author

Burkhardt, M.S., Foster, J.K., Laws, S.M., Baker, L.D., Craft, S., Gandy, S.E., Stuckey, B.G.A., Clarnette, R., Nolan, D., Hewson-Bower, B., Martins, R.N., Burkhardt, M.S., Foster, J.K., Laws, S.M., Baker, L.D., Craft, S., Gandy, S.E., Stuckey, B.G.A., Clarnette, R., Nolan, D., Hewson-Bower, B., and Martins, R.N.

Abstract

There is currently intense controversy regarding the use of hormone replacement therapy (HRT) in postmenopausal women, in relation to its therapeutic efficacy in Alzheimer's disease (AD). It has been suggested that the benefits of HRT may be modified by apolipoprotein E (APOE) genotype (the major genetic risk factor for AD). Here we report the findings of the first study designed to systematically explore the interaction of (a) oestrogen replacement therapy (ERT) and (b) possession of an ε4 allele of APOE on specific elements of episodic learning and memory that are commonly used indices of age-related cognitive decline. This data represents a cross-sectional analysis of the interaction of ERT and APOE genotype on learning and memory in a cohort of 181 healthy postmenopausal women [ERT users (n = 101, mean age 65.40 ± 6.34); ERT non-users (n = 80, mean age 67.03 ± 6.80)] residing in Perth, Western Australia. The highest level of learning (trials 2-5; P < 0.05) and memory (e.g. total number of items recalled; P < 0.05) performance was observed in women taking ERT who were not carriers of the APOE ε4 allele. APOEε4 carriers receiving ERT performed no better on episodic memory testing than APOE ε4 carriers who were not receiving ERT. These cognitive differences related to genetic profile, were noted on both recall and recognition (P = 0.005) tests of memory. The findings have significance for evaluating whether and when ERT may be clinically indicated. Specifically, ERT may benefit the cognitive functioning of women not carrying the APOE ε4 allele.

Published
2004

33. Cognitive impairment, physical disability and depressive symptoms in older diabetic patients: the Fremantle Cognition in diabetes study

Author

Bruce, D., Bruce, D., Casey, G., Grange, V., Clarnette, R., Almeida, O., Foster, Jonathan, Ives, F., Davis, T., Bruce, D., Bruce, D., Casey, G., Grange, V., Clarnette, R., Almeida, O., Foster, Jonathan, Ives, F., and Davis, T.

Abstract

Objective: To determine whether the prevalence of dementia, depression and/or disability in older diabetic subjects warrants an active screening approach by diabetes health care workers. Patients and methods: The initial 223 members of a cohort of 529 eligible diabetic subjects, aged 70 years or over, were screened for cognitive impairment (using the Mini-Mental State Examination (MMSE) and Informant Questionnaire for Cognitive Decline in the Elderly (IQCODE)), physical impairments and depressive symptoms. Results: Virtually all subjects were community-dwelling (99%) and mobile (86%) and relatively few had moderate or severe deficits in activities of daily living (ADL) (17.5%). The prevalences of cognitive impairment and probable dementia estimated from the screening tests were high (range 10.8–17.5%) compared with population studies. Any deficit with ADL was reported by 53% of the subjects and common problems included urinary and faecal incontinence. Scores consistent with clinical depression were reported by 14.2% of the sample but 50.2% of the remainder reported one or more depressive symptoms below the cut-off point for clinical depression. Only 36% of the study subjects were free of deficits in any domain. Conclusions: Community-living older diabetic subjects have high rates of cognitive impairment, deficits in physical function and depressive symptomatology suggesting that screening programs for functional impairments and depression may be beneficial in health care systems that manage older diabetic patients.

Published
2003

43. Neurological soft signs are associated with APOE genotype, age and cognitive performance.

Author

Lautenschlager, N. T., Jing-Shan Wu, Laws, S. M., Almeida, O. P., Clarnette, R. M., Joesbury, K., Wagenpfeil, S., Martins, G., Paton, A., Gandy, S. E., Förstl, H., and Martins, R. N.

Subjects
NEURODEGENERATION, MEMORY, COGNITION, APOLIPOPROTEIN E, MENTAL health
Abstract

Neurodegeneration is associated with increased frequency of neurological soft signs (NSS). We designed the present study to investigate the association between NSS and subjective memory complaints, cognitive function and apolipoprotein E genotype in a community-dwelling sample of volunteers participating in an ongoing longitudinal program investigating predictors of cognitive decline. NSS were found to be associated with apolipoprotein E (APOE) ℇ4 genotype (p = 0.015), age (p = 0.012) and poor cognitive performance, as assessed by the Mini Mental State Examination (p = 0.053). There was no significant difference between subjects with and without memory complaints in relation to the frequency of NSS (p = 0.130). The association with age and the APOE ℇ4 genotype suggests that the systematic investigation of NSS may contribute to identify subjects at risk of clinically significant cognitive decline in later life. [ABSTRACT FROM AUTHOR]

Published
2005
Full Text
View/download PDF

44. Oestrogen replacement therapy may improve memory functioning in the absence of APOE epsilon4.

Author

Burkhardt, M. S., Foster, J. K., Laws, S. M., Baker, L. D., Craft, S., Gandy, S. E., Stuckey, B. G. A., Clarnette, R., Nolan, D., Hewson-Bower, B., and Martins, R. N.

Subjects
ESTROGEN replacement therapy, MEMORY, APOLIPOPROTEIN E, HORMONE therapy, ALZHEIMER'S disease
Abstract

There is currently intense controversy regarding the use of hormone replacement therapy (HRT) in postmenopausal women, in relation to its therapeutic efficacy in Alzheimer's disease (AD). It has been suggested that the benefits of HRT may be modified by apolipoprotein E (APOE) genotype (the major genetic risk factor for AD). Here we report the findings of the first study designed to systematically explore the interaction of (a) oestrogen replacement therapy (ERT) and (b) possession of an epsilon4 allele of APOE on specific elements of episodic learning and memory that are commonly used indices of age-related cognitive decline. This data represents a cross-sectional analysis of the interaction of ERT and APOE genotype on learning and memory in a cohort of 181 healthy postmenopausal women [ERT users (n = 101, mean age 65.40 +/- 6.34); ERT non-users (n = 80, mean age 67.03 +/- 6.80)] residing in Perth, Western Australia. The highest level of learning (trials 2-5; P < 0.05) and memory (e.g. total number of items recalled; P < 0.05) performance was observed in women taking ERT who were not carriers of the APOE epsilon4 allele. APOEepsilon4 carriers receiving ERT performed no better on episodic memory testing than APOE epsilon4 carriers who were not receiving ERT. These cognitive differences related to genetic profile, were noted on both recall and recognition (P = 0.005) tests of memory. The findings have significance for evaluating whether and when ERT may be clinically indicated. Specifically, ERT may benefit the cognitive functioning of women not carrying the APOE epsilon4 allele. [ABSTRACT FROM AUTHOR]

Published
2004
Full Text
View/download PDF

49. High content, multi-parameter analyses in buccal cells to identify alzheimer’s disease

Author

François, M., Fenech, M. F., Thomas, P., Hor, M., Rembach, A., Martins, R. N., Rainey-Smith, S. R., Masters, C. L., Ames, D., Rowe, C. C., Lance Macaulay, S., Hill, A. F., Leifert, W. R., Appannah, A., Barnes, M., Barnham, K., Bedo, J., Bellingham, S., Bon, L., Bourgeat, P., Brown, B., Buckley, R., Burnham, S., Bush, A., Chandler, G., Chen, K., Clarnette, R., Collins, S., Cooke, I., Cowie, T., Cox, K., Cuningham, E., Cyarto, E., Dang, P. A. V., Darby, D., Desmond, P., Doecke, J., Dore, V., Downing, H., Dridan, B., Duesing, K., Fahey, M., Farrow, M., Faux, N., Fenech, M., Fernandez, S., Fernando, B., Fowler, C., Francois, M., Fripp, J., Frost, S., Gardener, S., Gibson, S., Graham, P., Gupta, V., Hansen, D., Harrington, K., Hill, A., Hone, E., Horne, M., Huckstepp, B., Jones, A., Jones, G., Kamer, A., Kanagasingam, Y., Keam, L., Kowalczyk, A., Krivdic, B., Lam, C. P., Lamb, F., Lautenschlager, N., Laws, S., Leifert, W., Lenzo, N., Leroux, H., Lftikhar, F., Li, Q. -X, Lim, F., Lim, L., Lockett, L., Lucas, K., Mano, M., Marczak, C., Martins, G., Maruff, P., Matsumoto, Y., Bird, S., Mcbride, S., Mckay, R., Mulligan, R., Nash, T., Nigro, J., O Keefe, G., Ong, K., Parker, B., Pedrini, S., Peiffer, J., Pejoska, S., Penny, L., Perez, K., Pertile, K., Phal, P., Porter, T., Rainey-Smith, S., Raniga, P., Restrepo, C., Riley, M., Roberts, B., Robertson, J., Rodrigues, M., Rooney, A., Rumble, R., Ryan, T., Salvado, O., Samuel, M., Saunders, I., Savage, G., Silbert, B., Sohrabi, H., Syrette, J., Cassandra Szoeke, Taddei, K., Taddei, T., Tan, S., Tegg, M., Trivedi, D., Trounson, B., Veljanovski, R., Verdile, G., Villemagne, V., Volitakis, I., Vockler, C., Vovos, M., Vrantsidis, F., Walker, S., Watt, A., Weinborn, M., Wilson, B., Woodward, M., Yastrubetskaya, O., Yates, P., Zhang, P., Chatterjee, P., Creegan, R., Ruyck, K., Ding, H., Groth, D., Head, R., Krause, D., Lachovitzki, R., Lim, Y. Y., Lintern, T., Mondal, A., Nuttall, S., O Callaghan, N., Osborne, L., Pang, C., Patten, G., Tuckfield, A., Varghese, J., Wilson, A., and Zhang, Q.

Catalog

Books, media, physical & digital resources
See catalog results