Recent Progress in Alzheimer’s Disease Research, Part 3: Diagnosis and Treatment

Hane, Francis; Robinson, Morgan; Lee, Brenda Yasie; Bai, Owen; Leonenko, Zoya; Albert, Mitchell S.

doi:10.3233/jad-160907

Cited by 168 publications

(135 citation statements)

References 133 publications

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“…Given the strong evidence supporting the role of Aβ accumulation in the AD brain [1], failure of anti‐Aβ agents does not necessarily disprove the amyloid hypothesis but perhaps suggests that Aβ load reduction alone may not be enough to reverse the neurite dystrophy and dementia of AD [4]. Because Aβ plaque deposition occurs decades before clinical AD [5], therapeutic agents that enhance the repair of dystrophic neurites after plaque reduction may aid in the reversal of dementia. Therefore, a therapy that combines Aβ load reduction with reversal of neuronal damage may yield cognitive improvement in AD.…”

Section: Introductionmentioning

confidence: 99%

Hematologic safety of chronic brain‐penetrating erythropoietin dosing in APP/PS1 mice

Sun

Yang

Whitman

et al. 2019

A&D Transl Res & Clin Interv

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Introduction Low blood‐brain barrier (BBB) penetration and hematopoietic side effects limit the therapeutic development of erythropoietin (EPO) for Alzheimer's disease (AD). A fusion protein of EPO and a chimeric monoclonal antibody targeting the mouse transferrin receptor (cTfRMAb) has been engineered. The latter drives EPO into the brain via receptor‐mediated transcytosis across the BBB and increases its peripheral clearance to reduce hematopoietic side effects of EPO. Our previous work shows the protective effects of this BBB‐penetrating EPO in AD mice but hematologic effects have not been studied. Herein, we investigate the hematologic safety and therapeutic effects of chronic cTfRMAb‐EPO dosing, in comparison to recombinant human EPO (rhu‐EPO), in AD mice. Methods Male APPswe PSEN1dE9 (APP/PS1) mice (9.5 months) were treated with saline (n = 11), and equimolar doses of cTfRMAb‐EPO (3 mg/kg, n = 7), or rhu‐EPO (0.6 mg/kg, n = 9) 2 days/week subcutaneously for 6 weeks, compared to saline‐treated wild‐type mice (n = 10). At 6 weeks, exploration and memory were assessed, and mice were sacrificed at 8 weeks. Spleens were weighed, and brains were evaluated for amyloid beta (Aβ) load and synaptophysin. Blood was collected at 4, 6 and 8 weeks for a complete blood count and white blood cells differential. Results cTfRMAb‐EPO transiently increased reticulocyte counts after 4 weeks, followed by normalization of reticulocytes at 6 and 8 weeks. rhu‐EPO transiently increased red blood cell count, hemoglobin and hematocrit, and significantly decreased mean corpuscular volume and reticulocytes at 4 weeks, which remained low at 6 weeks. At 8 weeks, a significant decline in red blood cell indices was observed with rhu‐EPO treatment. Exploration and cognitive deficits were significantly worse in APP/PS1‐rhu‐EPO mice. Both cTfRMAb‐EPO and rhu‐EPO decreased 6E10‐positive brain Aβ load; however, cTfRMAb‐EPO and not rhu‐EPO selectively reduced brain Aβ1‐42 and elevated synaptophysin expression. Discussion Chronic treatment with cTfRMAb‐EPO results in better hematologic safety, behavioral, and therapeutic indices compared with rhu‐EPO, supporting the development of this BBB‐penetrable EPO analog for AD.

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Section: Introductionmentioning

confidence: 99%

Hematologic safety of chronic brain‐penetrating erythropoietin dosing in APP/PS1 mice

Sun

Yang

Whitman

et al. 2019

A&D Transl Res & Clin Interv

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“…Recent advances on the understanding of Alzheimer's disease genetics and molecular pathways have helped identifying novel cerebrospinal fluid and blood biomarkers, as well as the development of promising new therapies that are currently being tested . Among the promising therapies, are those which target Aβ production, direct targeting of Aβ and tau, and immunotherapy . Traditional preventive therapies, which improve brain circulation are still used to target Alzheimer's disease …”

Section: Research and Future Directionsmentioning

confidence: 99%

“…Among the promising therapies, are those which target Aβ production, direct targeting of Aβ and tau, and immunotherapy . Traditional preventive therapies, which improve brain circulation are still used to target Alzheimer's disease …”

Section: Research and Future Directionsmentioning

confidence: 99%

“…4,6 However, it has also showed that this causality is not linear, being rather more complex and involving multiple causes. 4,75 Recent advances on the understanding of Alzheimer's disease genetics and molecular pathways have helped identifying novel cerebrospinal fluid and blood biomarkers, 4,37,76 as well as the development of promising new therapies that are currently being tested. 31,66 Among the promising therapies, are those which target A production, direct targeting of A and tau, and immunotherapy.…”

Section: What Are the Most Promising Strategies?mentioning

confidence: 99%

“…31,66 Among the promising therapies, are those which target A production, direct targeting of A and tau, and immunotherapy. 37,76 Traditional preventive therapies, which improve brain circulation are still used to target Alzheimer's disease. 76 With regard to the clinical management of Alzheimer's disease, only minor progress has been reported to improve the quality of life for patients with Alzheimer's disease and their caregivers.…”

Section: What Are the Most Promising Strategies?mentioning

confidence: 99%

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Oral health care for patients with Alzheimer's disease: An update

Marchini

Ettinger

Caprio

et al. 2019

Special Care in Dentistry

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Alzheimer's disease and related disorders (ADRD) are among the age‐associated chronic conditions that are most challenging to health care systems around the globe, as patients with dementia require full‐time, intensive care for multiple years. Oral health care is negatively impacted by cognitive decline, and consequently poor oral health is common among people with ADRD. Poor oral health status is linked with many undesirable consequences for the well‐being of people with ADRD, from excruciating local pain to life‐threatening conditions, as aspiration pneumonia. In this paper, the authors provide an update on the most current concepts about Alzheimer's disease epidemiology, etiology, and management, current oral health care for patients with Alzheimer's disease, oral health promotion strategies for this population, as well as current research and future direction for improving oral health care for patients with Alzheimer's disease. It concludes that oral health care should be included in the patient's routine health care as early as possible in the progression of Alzheimer's disease for preventing rapid oral health deterioration. Establishing oral hygiene routines and providing dental treatment that is customized to the patients’ individual needs and disease stage are important to achieve good oral health outcomes and prevent quality of life decline.

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Long COVID-19 Neurological and Psychological Claims: Assessment Guidelines

Hirsch¹,

Mandel²,

Kertay³

et al. 2022

AMA Guides® Newsletter

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Post–severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) (coronavirus disease 2019 [COVID-19]) conditions are referred to by a wide range of names, including long COVID, post-acute COVID-19, long-term effects of COVID, post-acute COVID syndrome, chronic COVID, long-haul COVID, late sequelae, and others, as well as the research term, post-acute sequelae of SARS-CoV-2 infection (PASC). Symptoms may include difficulty thinking or concentrating, fatigue, depression, anxiety, and other complaints. The results of studies are clouded by self-reports, lack of objective cognitive data, misattribution, and ill-defined psychological issues. Prospective cohort studies with objective assessment are needed to clarify the impact of COVID-19. While we do not dismiss the presence of long COVID or chronic COVID-19 symptoms lasting beyond a typically expected viral respiratory-transmitted syndrome, neither do we uncritically accept such a syndrome in all those who were diagnosed as having COVID-19, especially in those whose initial presentation was asymptomatic or mild. Evaluators must be astute and perform unbiased, thorough assessments and focus on objective findings while carefully assessing the potential for confounding or alternate conditions.

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Recent Progress in Alzheimer’s Disease Research, Part 3: Diagnosis and Treatment

Cited by 168 publications

References 133 publications

Hematologic safety of chronic brain‐penetrating erythropoietin dosing in APP/PS1 mice

Hematologic safety of chronic brain‐penetrating erythropoietin dosing in APP/PS1 mice

Oral health care for patients with Alzheimer's disease: An update

Long COVID-19 Neurological and Psychological Claims: Assessment Guidelines

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