Thursday, April 07, 2022

Epidemiological and Clinical Characteristics of Sporadic Creutzfeldt–Jakob Disease: A Retrospective Study in Eastern China

Epidemiological and Clinical Characteristics of Sporadic Creutzfeldt–Jakob Disease: A Retrospective Study in Eastern China

Shuo Feng1Xinjing Zhao2Xueying Zhou3Xiang Ye2Xiaolin Yu2Wei Jiang2Yu Deng4Shengnian Zhou1Lin Ma2Peiyan Shan2 and Guoyu Zhou2*
  • 1Department of Neurology, Qilu Hospital of Shandong University, Jinan, China
  • 2Department of Geriatric Neurology, Qilu Hospital of Shandong University, Jinan, China
  • 3Department of Physical Medicine and Rehabilitation, Qilu Hospital of Shandong University, Jinan, China
  • 4Department of Environmental Health, School of Public Health, China Medical University, Shenyang, China

Objective: We aimed to characterize the epidemiological and clinical characteristics of sporadic Creutzfeldt–Jakob disease (sCJD) in eastern China in this retrospective study.

Methods: This study enrolled 67 patients with sCJD hospitalized in a grade-A tertiary hospital in eastern China from January 2010 to January 2020. Demographic data, clinical symptoms, brain magnetic resonance imaging (MRI), electroencephalogram (EEG), cerebrospinal fluid (CSF) 14-3-3 protein test, polymerase chain reaction (PCR), and DNA sequence determination of genes were collected and analyzed.

Results: There were 62 patients with probable sCJD and 5 patients with possible sCJD. Male (28 cases) to female (39 cases) ratio was 1:1.39. Mean age at disease onset was 64.42 ± 9.00 years (range: 29–88 years), and mean survival time was 9.39 ± 12.58 months (range: 1–60 months for patients who received the follow-ups). The most common onset symptoms were dementia (49.25%), movement disorder (44.78%), and visual disturbance (22.39%), while the most frequent clinical manifestations were language disorders (74.63%), ataxia (70.15%), and myoclonus (70.15%). The positive rates of brain MRI abnormalities, 14-3-3 protein in CSF, and periodic sharp wave complexes (PSWCs) on EEG were 84.90, 68.00, and 46.03%, respectively. The 14-3-3 protein positive (p = 0.033) and PSWCs on EEG (p = 0.020) acted as the favorable and unfavorable factor for over 1 year of survival time, respectively.

Conclusions: There were some differences in epidemiological and clinical characteristics among patients in China and those of other countries. The prognosis and its influencing factors were relatively unexplored in China. The mean survival time of Chinese patients was longer than that of Caucasian patients but shorter than that of Japanese patients. The 14-3-3 protein in CSF and PSWCs on EEG were both closely related to the survival time. It is necessary to promote autopsy or biopsy to better understand sCJD in China.

Introduction

Prion diseases (PrDs), also known as transmissible spongiform encephalopathies (TSEs), are a group of rare, rapidly progressive and fatal central nervous system diseases attacking humans and animals. According to the modes of human PrDs, PrDs can be classified into three different categories: sporadic (spontaneous), genetic (familial, inherited), and acquired (infectious, transmitted). The sporadic type, the most prevalent one (85–90%), consists of sporadic Creutzfeldt–Jakob disease (sCJD), rare entities of sporadic fatal insomnia, and variably protease-sensitive prionopathy (VPSPr) (12). sCJD is generally regarded as a spontaneous neurodegenerative illness, arising either from templated misfolding and protein conformation change of PrPC (normal brain prion-related protein) or spontaneous somatic mutation of PRNP (gene encoding the PrPC). sCJD is clinically characterized by rapidly progressive dementia with ataxia, myoclonus, or other neurologic symptoms (34) and neuropathologically represented by the presence of aggregates of abnormal prion protein, spongiform change, neuronal loss, and gliosis (5). At least six molecular pathological subtypes are classified by genotypes of PRNP codon 129 and protease cleavage sites of PrPSc (misfolded disease-causing forms), which includes MM1, MV1, VV1, MM2, MV2, and VV2. They are responsible for the diversity of clinical characteristics like onset age, survival time, and symptoms (67).

sCJD is a globally distributed disease. The identification of disease phenotype spectrum has greatly increased the possibility of early diagnosis of sCJD subtype specifically, which is also the foundation of developing effective treatments. In China, the CJD surveillance program supported by the Chinese Center for Disease Control and Prevention (CCDC) was conducted since 2006. sCJD cases (261) were reported nationwide from 2006 to 2010, with a higher number of cases in the east compared with those in other regions (8). However, the prevalence of sCJD has been rarely reported in the past decade in China. Besides, clinical features such as gender ratio and survival time are not consistent in several Chinese studies. Data on the prognosis of Chinese sCJD patients is even more deficient (814), and only one study had analyzed the factors affecting it (11). It is urgent to understand the current situation of sCJD in China. Here we presented a retrospective study on the epidemiologic and clinical characteristics and the prognoses of 67 sCJD patients in eastern China to raise awareness of this rare neurodegenerative disease.

Materials and Methods

snip...

Discussion

In the current study, we retrospectively analyzed the demographic and clinical features of 67 sCJD patients in eastern China, and 43 of them received follow-ups. By the end of the study, 39 follow-up patients had died. Generally speaking, though PrDs are considered rare, the number of sCJD cases diagnosed in our hospital has been on the rise over the past 10 years. This may be attributed to the aging population, increasing number of patients admitted to hospital, and improved clinician awareness of the disease. However, the number of cases peaked in 2017 and has since declined mildly. It is for sure that the total number of inpatients from the department of neurology in our hospital has been increasing from 2010 to 2019. Given that the number of CJD cases nationwide in the recent 5 years has not been published, and other Chinese single-center study have not paid attention to the trend of the number of the patients, whether this trend is consistent with the national situation remains unknown.

In this study, we found that there were more female than male sCJD patients, and the female-to-male ratio was 1.39. Two studies of Chinese patients were consistent with our findings, in which the number of females predominated (1012), but two other studies had reported a higher proportion of males, where the female-to-male ratio was 0.82 and 0.79, respectively (814). Because of small sample size and various nationalities in China, there might be biases in those results. A convincing gender ratio of sCJD patients in China requires demographic data of multicenter or population-based studies in the future. According to Japanese national sCJD surveillance data from 2001 to 2010, the ratio of female to male was 1.15 (16). In a research with 2,451 pathologically confirmed sCJD patients enrolled by the European Creutzfeldt–Jakob Disease Network (EUROCJD), which covered several European countries, Canada, and Australia, the ratio of female to male was 1.18 (7). In contrast, the data of 116 sCJD cases from the United States demonstrated that the female-to-male ratio was 0.49 (17). It is worth noting that this American study included patients of multiple races including Whites, Blacks, and American Indians. Race, population structure, molecular pathological subtype pattern, and the gender difference in economic status could partly contribute to the disparate ratios by countries. Further researches are required to investigate the exact reasons by controlling multiple factors. What is more, adequate sample size is indispensable in that the patient numbers of Chinese studies are much less than that in other countries.

The mean age of disease onset in this study (64.42 years old) was comparable with the findings from Korea (65.5 years) (18), Japan (65.5 years) (19), the United States (66.15 years), (20) and Europe (66 years) (21), but higher than that of a few Chinese patient groups [58 years (14) 60.3 years (9)]. Another two surveys in China have produced results essentially in agreement with ours at the median onset age, which was 64 years in our study (811). According to these reported Chinese studies, most of suspected patients were not tested for PRNP gene to rule out genetic Creutzfeldt–Jakob disease (891114), which might affect the results and analysis of the study. Similarly, there were two patients younger than 30 years old in our study. Although these two patients met the criteria for clinical diagnosis of sCJD, they were not eventually diagnosed by pathological examination, which may also have an impact on the result. At the same time, considering that the different regional demographic features might play a role in the heterogeneity of onset ages among domestic studies, more accurate onset age remains to be verified by large national surveys. Additionally, Kotkowski et al. found that age (66 ± 11.5 years) was correlated with sCJD onset (20). As with many other neurodegenerative diseases, sCJD generally occurs in late adulthood.

So far, no effective treatment has been developed for sCJD, which remains uniformly fatal. In our study, the mean survival time was 9.39 months, and 72.09% of the sCJD patients had a survival time <1 year. Similarly, other researches in China showed that mean survival time ranged from 6.1 to 11.6 months, and 1-year mortality was 68.50–74.00% (111314). We also found that 14-3-3 protein and PSWCs acted as the favorable and unfavorable factor for over 1 year of survival time, respectively. The same predictive effect of PSWCs was also observed in two European large-scale studies, in which over 2,000 pathologically definite sCJD cases were incorporated (722). However, some studies have found that 14-3-3 protein was correlated with a shorter survival time (72124). The possible reasons for this discrepancy may be as follows: first of all, there are only two 14-3-3 protein-positive patients in this study, whose survival times were <1 year. Considering the small sample size and related uncertainties, our findings need to be further validated by large-scale studies. Second, the survival time is usually not determined by a single factor, which is why Llorens et al. have set up a multifactor predictive model (21). To our knowledge, previous study objects were Caucasians, but no Chinese researchers have explored the relationship between CSF biomarkers and survival time. Different races, regional environments, molecular subtypes and some relevant unknown factors may partly explain our different findings. Last but not the least, pathological examinations were not carried out in our patients, which could reduce the accuracy of diagnoses and then affect the results. Pocchiari et al. concluded that there was correlation between survival time and codon 129 type (22). The multinational study carried out by EUROCJD, whose research objects were mainly Caucasians, revealed that the mean survival time was only 5 months, and 85.8% of the cases died within 1 year. The MM, MV, and VV type of codon 129 accounted for 66.1, 17.0, and 16.9%, respectively (7). In Asia, almost all the sCJD patients were MM type (8911142527). MM type accounted for 97.0–100.0% of all sCJD patients according to previous Chinese studies, while others were all MV type (89111427), which was in agreement with our findings. However, due to the extreme paucity of pathological examination, PrPSc types of Chinese sCJD patients are unavailable till now. As a consequence, different distribution patterns of PRNP codon 129 types may be one of the reasons for the variations in survival time, and other possible reasons remain to be explored.

However, according to a Japanese report, the mean survival time and 1-year mortality was 15.7 months and 48.1%, respectively (26). By comparison, survival time of the patients is shorter in China, where the MM type is the majority in Japan, though (8111426). It should be noted that there is a proportion of Japanese patients with MM2 type, and nearly all of those survival time was more than 1 year, and some even reached 6 years (28). Additionally, the MM2 type can be further divided into MM2C and MM2T subtypes based on distinctive cortical and thalamic histopathology (229), and the MM2T subtype is also known as sporadic familial insomnia (sFI), which is relatively rare. Their mean survival time was comparable despite different races (2830). Studies also have shown that MM1 type patients had an obviously shorter media survival time of 4.0–9.0 months (731). However, the pathological classification of MM type is still not clear in China, which might be the main reason for the different survival time between Japanese and Chinese patients. More pathological results are needed to verify it. What is more, Iwasaki et al. found that tube feeding was an independent factor influencing total disease duration for MM1 type of sCJD (31), which also partly accounted for the longer survival time of Japanese patients (32). Future studies should be conducted by controlling possible interfering factors, such as regions, economic conditions, races, or molecular pathological subtypes, to find the exact factors that affect the course of disease.

The most common initial symptoms in our study were dementia, movement disorder, and visual disturbance, which were consistent with the results of other two centers in China (911). It was reported by a Japanese research that 55.10% of cases started from psychiatric symptoms such as dementia or sleeping difficulties (26). According to a German study of 492 sCJD patients, dementia was the most common initial symptom followed by cerebellar, visual, and psychiatric disturbances (33). An American study with 114 sCJD patients showed that cognitive symptoms, especially memory loss, were the most common manifestations (34). Despite the discrepancies in race, region and even molecular pathological types, dementia is the most frequent onset symptom in these patients. Most notably, 49.25% of our patients rapidly developed progressive dementia, almost all of whom had this symptom at the time of seeking medical treatments.

The diagnosis of sCJD is challenging. Only autopsy can make a definite diagnosis, but most diagnoses of sCJD are based on clinical manifestations and ancillary tests without specific biological markers. Biomarkers with high specificity and sensitivity are urgently needed to assist clinicians in diagnosing sCJD. The first biomarker identified for diagnosis was PSWCs on EEG, which was performed in 63 patients in our study. Only 29 (46.03%) of them showed positive results, but the sensitivity of PSWCs among the confirmed CJD patients was 55.7–64% (735). Since PSWCs usually occur in the late stages of the disease, the timing of test can also affect the positive rates. Serial EEG recordings are required for higher positive rates (3638). Furthermore, given that PSWCs are common in encephalopathies, metabolic disorders, dementias, and other diseases, the specificity is relatively low (353941). Another widely used biomarker was 14-3-3 protein in CSF. As a moderately sensitive biomarker (42), 14-3-3 protein showed a positive rate of 68.00% in our cases, not very prominent detecting efficiency. Compared with PSWCs and 14-3-3 protein, brain diffusion-weighted MRI has a higher diagnostic utility in sCJD, with a sensitivity ranging from 92 to 96% and a specificity of about 93 to 94% (4345). Further studies indicated that specific MRI abnormalities could serve as useful parameters for predicting the clinical course, such as those who have cortical plus basal ganglia hyperintensity on DWI tend to show symptoms of advanced stage (4647). The abnormal rate of brain MRI of our patients was 84.85%, which was a bit lower than that of studies with some defined patients (104244). One of the possible reasons is that our clinical diagnosis of sCJD is not conclusive without pathological inspections. In recent years, some of the newer diagnostic markers have also been explored; total (t)-tau protein in CSF was found to be superior to 14-3-3 protein and neurofilament light chain protein (NfL) as a biomarker with the highest sensitivity of 88.2–90.20% (48) and specificity of 74.5–78.9% (4950). The ratio of t-tau and phosphorylated-tau may be useful to distinguish patients with CJD from patients with other dementias (5152). In addition, a new PrPSc amplification assay, named real-time quaking-induced conversion (RT-QuIC), has also shown an overall diagnostic sensitivity of 82.1–92% and a specificity of 98.5–100% (495356), sometimes behind t-tau. Unfortunately, none of our patients had received the above two tests on account of technical limitations and examination costs. These problems could change with the deepening understanding and research of the disease.

Compared with nearly 100% in Austria (57), 68.7% in the United States (58), 66% in Germany (59), 60% in Australia (60), and 51% in Belgium (61), the autopsy rate is extremely low among Chinese patients due to the influence of traditional Chinese values. Besides, the fear and limited understanding of prion disease, as well as the restriction on the conditions of medical institutions, also affect autopsies on patients with this contagious neurodegenerative disease in China. Biopsy could not be performed smoothly and generally in China, either, which was confirmed by previous domestic literature (81013). Thus, their vast majority of molecular pathological subtypes remained unknown. To have a more accurate understanding of sCJD in China, the application of autopsy or biopsy in suspected patients is urgently needed.

This study described and analyzed the epidemiological and clinical characteristics of sCJD patients in eastern China systematically. Compared with most previous studies in China, we have gotten a relatively detailed clinical characteristics and complete follow-up data, and conducted a thorough analysis of the relationship between the two. Moreover, in the absence of autopsy and biopsy, compared with to the only study that performed prognostic analysis (11), the newer clinical diagnostic criteria were applied here. Differences in gender, 14-3-3 protein, PSWCs, and contributing factors on survival time were revealed in Chinese patients for the first time. There are also several limitations in our study. First, the number of sCJD cases was relatively small, and CSF 14-3-3 protein and PRNP gene analysis were not performed in all cases. With the ongoing deep research work, the rate of CSF and gene testing for patients with prion disease would increase gradually, thus, raising the accuracy of sCJD diagnosis. Second, some patients were lost to follow-up, resulting in unknown prognoses. In future research, we will expand the sample size and conduct more intensive and longer-term follow-up observations. Third, although the primary diagnostic methods for sCJD are t-tau and RT-QuIC, rather than the 14-3-3 protein and PSWCs now, the first two were not performed in this study. Finally, pathological examination of brain tissue, which is crucial to diagnosis, was not carried out. Along with the further understanding of prion disease and the development of medical and economic conditions in China, this situation is expected to be improved.

Conclusions

In conclusion, the epidemiological and clinical characteristics in Chinese studies are inconsistent, and there are some differences when compared with other countries. The mean survival time of Chinese patients was longer than that of Caucasian patients but shorter than that of Japanese patients. This study found that 14-3-3 protein in CSF and PSWCs on EEG acted as the favorable and unfavorable factor for over 1 year of survival time of Chinese patients, respectively, which has not been reported in previous literature of China. With an extremely low autopsy rate of prion disease in China, it is necessary to promote autopsy or biopsy to better understand the incidence, clinical characteristics, and the effective factors for prognosis of sCJD or prion diseases. Systematic studies on genes, protein, pathology, and clinical phenotypes are needed for a deeper insight of this disease as well as other possible neurodegenerative diseases related to protein misfolding.

https://www.frontiersin.org/articles/10.3389/fneur.2021.700485/full

83rd General Session • Paris, 24–29 May 2015 Final Report 2015

1. The Director General publish the following List of Member Countries recognised as having a negligible BSE risk in accordance with Chapter 11.4. of the Terrestrial Code:

Argentina Australia Austria Belgium Brazil Bulgaria Chile Colombia Croatia Cyprus Czech Republic Denmark Estonia Finland France Hungary Iceland India Ireland Israel Italy Japan Korea (Rep. of) Latvia Liechtenstein Luxembourg Malta Netherlands New Zealand Norway Panama Paraguay Peru Portugal Singapore Slovakia Slovenia Sweden Switzerland United States of America Uruguay

2. The Director General publish the following List of Member Countries recognised as having a controlled BSE risk in accordance with Chapter 11.4. of the Terrestrial Code:

Canada Chinese Taipei Costa Rica Germany Greece Lithuania Mexico Nicaragua Poland Spain United Kingdom

3. The Director General publish the following List of Member Countries having a zone4 recognised as having a negligible BSE risk in accordance with Chapter 11.4. of the Terrestrial Code:

China (People’s Rep. of): a zone designated by the Delegate of China in a document addressed to the Director General in November 2013, consisting of the People’s Republic of China with the exclusion of Hong Kong and Macau.

AND

4. The Delegates of these Member Countries shall immediately notify the OIE Headquarters if BSE occurs in their countries or their territories.

https://www.oie.int/app/uploads/2021/03/a-fr-2015-public.pdf

https://www.oie.int/app/uploads/2021/05/a-r17-2021-bse.pdf

UPDATED OIE ATYPICAL BSE!

OIE Conclusions on transmissibility of atypical BSE among cattle

Given that cattle have been successfully infected by the oral route, at least for L-BSE, it is reasonable to conclude that atypical BSE is potentially capable of being recycled in a cattle population if cattle are exposed to contaminated feed. In addition, based on reports of atypical BSE from several countries that have not had C-BSE, it appears likely that atypical BSE would arise as a spontaneous disease in any country, albeit at a very low incidence in old cattle. In the presence of livestock industry practices that would allow it to be recycled in the cattle feed chain, it is likely that some level of exposure and transmission may occur. As a result, since atypical BSE can be reasonably considered to pose a potential background level of risk for any country with cattle, the recycling of both classical and atypical strains in the cattle and broader ruminant populations should be avoided. 


Annex 7 (contd) AHG on BSE risk assessment and surveillance/March 2019

34 Scientific Commission/September 2019

3. Atypical BSE

The Group discussed and endorsed with minor revisions an overview of relevant literature on the risk of atypical BSE being recycled in a cattle population and its zoonotic potential that had been prepared ahead of the meeting by one expert from the Group. This overview is provided as Appendix IV and its main conclusions are outlined below. With regard to the risk of recycling of atypical BSE, recently published research confirmed that the L-type BSE prion (a type of atypical BSE prion) may be orally transmitted to calves1 . In light of this evidence, and the likelihood that atypical BSE could arise as a spontaneous disease in any country, albeit at a very low incidence, the Group was of the opinion that it would be reasonable to conclude that atypical BSE is potentially capable of being recycled in a cattle population if cattle were to be exposed to contaminated feed. Therefore, the recycling of atypical strains in cattle and broader ruminant populations should be avoided.

The Group acknowledged the challenges in demonstrating the zoonotic transmission of atypical strains of BSE in natural exposure scenarios. Overall, the Group was of the opinion that, at this stage, it would be premature to reach a conclusion other than that atypical BSE poses a potential zoonotic risk that may be different between atypical strains.

4. Definitions of meat-and-bone meal (MBM) and greaves

snip...

REFERENCES

SNIP...END SEE FULL TEXT;


Atypical L-type BSE

Emerg Infect Dis. 2017 Feb; 23(2): 284–287. doi: 10.3201/eid2302.161416 PMCID: PMC5324790 PMID: 28098532

Oral Transmission of L-Type Bovine Spongiform Encephalopathy Agent among Cattle 


Our study clearly confirms, experimentally, the potential risk for interspecies oral transmission of the agent of L-BSE. In our model, this risk appears higher than that for the agent of classical BSE, which could only be transmitted to mouse lemurs after a first passage in macaques (14). We report oral transmission of the L-BSE agent in young and adult primates. Transmission by the IC route has also been reported in young macaques (6,7). A previous study of L-BSE in transgenic mice expressing human PrP suggested an absence of any transmission barrier between cattle and humans for this particular strain of the agent of BSE, in contrast to findings for the agent of classical BSE (9). Thus, it is imperative to maintain measures that prevent the entry of tissues from cattle possibly infected with the agent of L-BSE into the food chain.


 In most cases of naturally occurring atypical BSE identified so far, the animals were >8 years of age, except for 3 cases: 1 H-BSE and 1 L-BSE in Spain (1) and 1 H-BSE in Germany (12). Therefore, we cannot exclude the possibility that L-BSE developed sporadically/spontaneously.

Consumption of L-BSE–contaminated feed may pose a risk for oral transmission of the disease agent to cattle.


Atypical H-type BSE

Research Project: Pathobiology, Genetics, and Detection of Transmissible Spongiform Encephalopathies Location: Virus and Prion

Research Title: The agent of H-type bovine spongiform encephalopathy associated with E211K prion protein polymorphism transmits after oronasal challenge 

This study demonstrates that the H-type BSE agent is transmissible by the oronasal route. 

These results reinforce the need for ongoing surveillance for classical and atypical BSE to minimize the risk of potentially infectious tissues entering the animal or human food chains.


Research Project: Pathobiology, Genetics, and Detection of Transmissible Spongiform Encephalopathies

Location: Virus and Prion Research

Title: The agent of H-type bovine spongiform encephalopathy associated with E211K prion protein polymorphism transmits after oronasal challenge

Author item Greenlee, Justin item MOORE, S - Orise Fellow item WEST-GREENLEE, M - Iowa State University

Submitted to: Prion

Publication Type: Abstract Only

Publication Acceptance Date: 5/14/2018

Publication Date: 5/22/2018

Citation: Greenlee, J.J., Moore, S.J., West Greenlee, M.H. 2018. The agent of H-type bovine spongiform encephalopathy associated with E211K prion protein polymorphism transmits after oronasal challenge. Prion 2018, May 22-25, 2018, Santiago de Compostela, Spain. Paper No. P98, page 116. Interpretive Summary:

Technical Abstract: In 2006, a case of H-type bovine spongiform encephalopathy (BSE) was reported in a cow with a previously unreported prion protein polymorphism (E211K). The E211K polymorphism is heritable and homologous to the E200K mutation in humans that is the most frequent PRNP mutation associated with familial Creutzfeldt-Jakob disease. Although the prevalence of the E211K polymorphism is low, cattle carrying the K211 allele develop H-type BSE with a rapid onset after experimental inoculation by the intracranial route. The purpose of this study was to investigate whether the agents of H-type BSE or H-type BSE associated with the E211K polymorphism transmit to wild type cattle or cattle with the K211 allele after oronasal exposure. Wild type (EE211) or heterozygous (EK211) cattle were oronasally inoculated with either H-type BSE from the 2004 US H-type BSE case (n=3) or from the 2006 US H-type case associated with the E211K polymorphism (n=4) using 10% w/v brain homogenates. Cattle were observed daily throughout the course of the experiment for the development of clinical signs. At approximately 50 months post-inoculation, one steer (EK211 inoculated with E211K associated H-BSE) developed clinical signs including inattentiveness, loss of body condition, weakness, ataxia, and muscle fasciculations and was euthanized. Enzyme immunoassay confirmed that abundant misfolded protein was present in the brainstem, and immunohistochemistry demonstrated PrPSc throughout the brain. Western blot analysis of brain tissue from the clinically affected steer was consistent with the E211K H-type BSE inoculum. With the experiment currently at 55 months post-inoculation, no other cattle in this study have developed clinical signs suggestive of prion disease. This study demonstrates that the H-type BSE agent is transmissible by the oronasal route. These results reinforce the need for ongoing surveillance for classical and atypical BSE to minimize the risk of potentially infectious tissues entering the animal or human food chains.


P98 The agent of H-type bovine spongiform encephalopathy associated with E211K prion protein polymorphism transmits after oronasal challenge 

Greenlee JJ (1), Moore SJ (1), and West Greenlee MH (2) (1) United States Department of Agriculture, Agricultural Research Service, National Animal Disease Center, Virus and Prion Research Unit, Ames, IA, United States (2) Department of Biomedical Sciences, Iowa State University College of Veterinary Medicine, Ames, IA, United States. 

With the experiment currently at 55 months post-inoculation, no other cattle in this study have developed clinical signs suggestive of prion disease. This study demonstrates that the H-type BSE agent is transmissible by the oronasal route. 

These results reinforce the need for ongoing surveillance for classical and atypical BSE to minimize the risk of potentially infectious tissues entering the animal or human food chains. 

PRION CONFERENCE 2018 CONFERENCE ABSTRACT

Published: 23 June 2011

Experimental H-type bovine spongiform encephalopathy characterized by plaques and glial- and stellate-type prion protein deposits

The present study demonstrated successful intraspecies transmission of H-type BSE to cattle and the distribution and immunolabeling patterns of PrPSc in the brain of the H-type BSE-challenged cattle. TSE agent virulence can be minimally defined by oral transmission of different TSE agents (C-type, L-type, and H-type BSE agents) [59]. Oral transmission studies with H-type BSE-infected cattle have been initiated and are underway to provide information regarding the extent of similarity in the immunohistochemical and molecular features before and after transmission. In addition, the present data will support risk assessments in some peripheral tissues derived from cattle affected with H-type BSE.

References...END


2.3.2. New evidence on the zoonotic potential of atypical BSE and atypical scrapie prion strains

PLEASE NOTE;

2.3.2. New evidence on the zoonotic potential of atypical BSE and atypical scrapie prion strains

Olivier Andreoletti, INRA Research Director, Institut National de la Recherche Agronomique (INRA) – École Nationale Vétérinaire de Toulouse (ENVT), invited speaker, presented the results of two recently published scientific articles of interest, of which he is co-author:

‘Radical Change in Zoonotic Abilities of Atypical BSE Prion Strains as Evidenced by Crossing of Sheep Species Barrier in Transgenic Mice’ (MarinMoreno et al., 2020) and ‘The emergence of classical BSE from atypical/Nor98 scrapie’ (Huor et al., 2019).

In the first experimental study, H-type and L-type BSE were inoculated into transgenic mice expressing all three genotypes of the human PRNP at codon 129 and into adapted into ARQ and VRQ transgenic sheep mice. The results showed the alterations of the capacities to cross the human barrier species (mouse model) and emergence of sporadic CJD agents in Hu PrP expressing mice: type 2 sCJD in homozygous TgVal129 VRQ-passaged L-BSE, and type 1 sCJD in homozygous TgVal 129 and TgMet129 VRQ-passaged H-BSE. 


3.2.1.2 Non‐cervid domestic species

The remarkably high rate of natural CWD transmission in the ongoing NA epidemics raises the question of the risk to livestock grazing on CWD‐contaminated shared rangeland and subsequently developing a novel CWD‐related prion disease. This issue has been investigated by transmitting CWD via experimental challenge to cattle, sheep and pigs and to tg mouse lines expressing the relevant species PrP.

For cattle challenged with CWD, PrPSc was detected in approximately 40% of intracerebrally inoculated animals (Hamir et al., 2005, 2006a, 2007). Tg mice expressing bovine PrP have also been challenged with CWD and while published studies have negative outcomes (Tamguney et al., 2009b), unpublished data provided for the purposes of this Opinion indicate that some transmission of individual isolates to bovinised mice is possible (Table 1).

In small ruminant recipients, a low rate of transmission was reported between 35 and 72 months post‐infection (mpi) in ARQ/ARQ and ARQ/VRQ sheep intracerebrally challenged with mule deer CWD (Hamir et al., 2006b), while two out of two ARQ/ARQ sheep intracerebrally inoculated with elk CWD developed clinical disease after 28 mpi (Madsen‐Bouterse et al., 2016). However, tg mice expressing ARQ sheep PrP were resistant (Tamguney et al., 2006) and tg mice expressing the VRQ PrP allele were poorly susceptible to clinical disease (Beringue et al., 2012; Madsen‐Bouterse et al., 2016). In contrast, tg mice expressing VRQ sheep PrP challenged with CWD have resulted in highly efficient, life‐long asymptomatic replication of these prions in the spleen tissue (Beringue et al., 2012).

A recent study investigated the potential for swine to serve as hosts of the CWD agent(s) by intracerebral or oral challenge of crossbred piglets (Moore et al., 2016b, 2017). Pigs sacrificed at 6 mpi, approximately the age at which pigs reach market weight, were clinically healthy and negative by diagnostic tests, although low‐level CWD agent replication could be detected in the CNS by bioassay in tg cervinised mice. Among pigs that were incubated for up to 73 mpi, some gave diagnostic evidence of CWD replication in the brain between 42 and 72 mpi. Importantly, this was observed also in one orally challenged pig at 64 mpi and the presence of low‐level CWD replication was confirmed by mouse bioassay. The authors of this study argued that pigs can support low‐level amplification of CWD prions, although the species barrier to CWD infection is relatively high and that the detection of infectivity in orally inoculated pigs with a mouse bioassay raises the possibility that naturally exposed pigs could act as a reservoir of CWD infectivity.


Very low oral exposure to prions of brain or saliva origin can transmit chronic wasting disease

Nathaniel D. Denkers ,Clare E. Hoover ,Kristen A. Davenport,Davin M. Henderson,Erin E. McNulty,Amy V. Nalls,Candace K. Mathiason,Edward A. Hoover 

Published: August 20, 2020


We report that oral exposure to as little as 300 nanograms (ng) of CWD-positive brain or to saliva containing seeding activity equivalent to 300 ng of CWD-positive brain, were sufficient to transmit CWD disease. This was true whether the inoculum was administered as a single bolus or divided as three weekly 100 ng exposures. However, when the 300 ng total dose was apportioned as 10, 30 ng doses delivered over 12 weeks, no infection occurred. While low-dose exposures to prions of brain or saliva origin prolonged the time from inoculation to first detection of infection, once infection was established, we observed no differences in disease pathogenesis. These studies suggest that the CWD minimum infectious dose approximates 100 to 300 ng CWD-positive brain (or saliva equivalent), and that CWD infection appears to conform more with a threshold than a cumulative dose dynamic.


TUESDAY, SEPTEMBER 07, 2021
Atypical Bovine Spongiform Encephalopathy BSE OIE, FDA 589.2001 FEED REGULATIONS, and Ingestion Therefrom



Bovine Spongiform Encephalopathy BSE TSE Prion Origin USA?


WEDNESDAY, JANUARY 12, 2022 

Bovine Spongiform Encephalopathy BSE TSE Prion Origin USA, what if?


PLOS ONE Journal 

*** Singeltary reply ; Molecular, Biochemical and Genetic Characteristics of BSE in Canada Singeltary reply ;


IBNC Tauopathy or TSE Prion disease, it appears, no one is sure 

Terry S. Singeltary Sr., 03 Jul 2015 at 16:53 GMT

***however in 1 C-type challenged animal, Prion 2015 Poster Abstracts S67 PrPsc was not detected using rapid tests for BSE.

***Subsequent testing resulted in the detection of pathologic lesion in unusual brain location and PrPsc detection by PMCA only.

*** IBNC Tauopathy or TSE Prion disease, it appears, no one is sure ***


MONDAY, NOVEMBER 30, 2020 

***> REPORT OF THE MEETING OF THE OIE SCIENTIFIC COMMISSION FOR ANIMAL DISEASES Paris, 9–13 September 2019 BSE, TSE, PRION

see updated concerns with atypical BSE from feed and zoonosis...terry


WEDNESDAY, DECEMBER 8, 2021 

Importation of Sheep, Goats, and Certain Other Ruminants AGENCY: Animal APHIA, USDA, FINAL RULE [Docket No. APHIS–2009–0095] RIN 0579–AD10 


WEDNESDAY, MARCH 24, 2021 

USDA Animal and Plant Health Inspection Service 2020 IMPACT REPORT BSE TSE Prion Testing and Surveillance MIA 


THURSDAY, AUGUST 20, 2020 

Why is USDA "only" BSE TSE Prion testing 25,000 samples a year? 


SUNDAY, MARCH 21, 2021 

Investigation Results of Texas Cow That Tested Positive for Bovine Spongiform Encephalopathy (BSE) Aug. 30, 2005 Singeltary's Regiew 2021 


TUESDAY, DECEMBER 21, 2021 

OIE-WAHIS CANADA atypical BSE type H Bovine spongiform encephalopathy


SATURDAY, DECEMBER 18, 2021 

CFIA Canada Alberta Laboratory detection of atypical bovine spongiform encephalopathy


THURSDAY, MARCH 31, 2022 

EFSA ONE Conference 2022 Chronic Wasting Disease CWD TSE PrP of Cervid and Zoonosis Zoonotic Transmission Singeltary Submission


TUESDAY, MARCH 29, 2022 

OIE Agent causing chronic wasting disease (CWD) TSE Prion of Cervid



***Moreover, sporadic disease has never been observed in breeding colonies or primate research laboratories, most notably among hundreds of animals over several decades of study at the National Institutes of Health25, and in nearly twenty older animals continuously housed in our own facility.***

Even if the prevailing view is that sporadic CJD is due to the spontaneous formation of CJD prions, it remains possible that its apparent sporadic nature may, at least in part, result from our limited capacity to identify an environmental origin.

https://www.nature.com/articles/srep11573 

O.05: Transmission of prions to primates after extended silent incubation periods: Implications for BSE and scrapie risk assessment in human populations 
Emmanuel Comoy, Jacqueline Mikol, Valerie Durand, Sophie Luccantoni, Evelyne Correia, Nathalie Lescoutra, Capucine Dehen, and Jean-Philippe Deslys Atomic Energy Commission; Fontenay-aux-Roses, France 

Prion diseases (PD) are the unique neurodegenerative proteinopathies reputed to be transmissible under field conditions since decades. The transmission of Bovine Spongiform Encephalopathy (BSE) to humans evidenced that an animal PD might be zoonotic under appropriate conditions. Contrarily, in the absence of obvious (epidemiological or experimental) elements supporting a transmission or genetic predispositions, PD, like the other proteinopathies, are reputed to occur spontaneously (atpical animal prion strains, sporadic CJD summing 80% of human prion cases). 

Non-human primate models provided the first evidences supporting the transmissibiity of human prion strains and the zoonotic potential of BSE. Among them, cynomolgus macaques brought major information for BSE risk assessment for human health (Chen, 2014), according to their phylogenetic proximity to humans and extended lifetime. We used this model to assess the zoonotic potential of other animal PD from bovine, ovine and cervid origins even after very long silent incubation periods. 

*** We recently observed the direct transmission of a natural classical scrapie isolate to macaque after a 10-year silent incubation period, 

***with features similar to some reported for human cases of sporadic CJD, albeit requiring fourfold long incubation than BSE. Scrapie, as recently evoked in humanized mice (Cassard, 2014), 

***is the third potentially zoonotic PD (with BSE and L-type BSE), 

***thus questioning the origin of human sporadic cases. 

We will present an updated panorama of our different transmission studies and discuss the implications of such extended incubation periods on risk assessment of animal PD for human health. 

=============== 

***thus questioning the origin of human sporadic cases*** 

=============== 

***our findings suggest that possible transmission risk of H-type BSE to sheep and human. Bioassay will be required to determine whether the PMCA products are infectious to these animals. 

============== 

https://prion2015.files.wordpress.com/2015/05/prion2015abstracts.pdf 

***Transmission data also revealed that several scrapie prions propagate in HuPrP-Tg mice with efficiency comparable to that of cattle BSE. While the efficiency of transmission at primary passage was low, subsequent passages resulted in a highly virulent prion disease in both Met129 and Val129 mice. 

***Transmission of the different scrapie isolates in these mice leads to the emergence of prion strain phenotypes that showed similar characteristics to those displayed by MM1 or VV2 sCJD prion. 

***These results demonstrate that scrapie prions have a zoonotic potential and raise new questions about the possible link between animal and human prions. 

http://www.tandfonline.com/doi/abs/10.1080/19336896.2016.1163048?journalCode=kprn20 

PRION 2016 TOKYO

Saturday, April 23, 2016

SCRAPIE WS-01: Prion diseases in animals and zoonotic potential 2016

Prion. 10:S15-S21. 2016 ISSN: 1933-6896 printl 1933-690X online

Taylor & Francis

Prion 2016 Animal Prion Disease Workshop Abstracts

WS-01: Prion diseases in animals and zoonotic potential

Transmission of the different scrapie isolates in these mice leads to the emergence of prion strain phenotypes that showed similar characteristics to those displayed by MM1 or VV2 sCJD prion. 

These results demonstrate that scrapie prions have a zoonotic potential and raise new questions about the possible link between animal and human prions. 

http://www.tandfonline.com/doi/abs/10.1080/19336896.2016.1163048?journalCode=kprn20

Title: Transmission of scrapie prions to primate after an extended silent incubation period) 

*** In complement to the recent demonstration that humanized mice are susceptible to scrapie, we report here the first observation of direct transmission of a natural classical scrapie isolate to a macaque after a 10-year incubation period. Neuropathologic examination revealed all of the features of a prion disease: spongiform change, neuronal loss, and accumulation of PrPres throughout the CNS. 

*** This observation strengthens the questioning of the harmlessness of scrapie to humans, at a time when protective measures for human and animal health are being dismantled and reduced as c-BSE is considered controlled and being eradicated. 

*** Our results underscore the importance of precautionary and protective measures and the necessity for long-term experimental transmission studies to assess the zoonotic potential of other animal prion strains. 

http://www.ars.usda.gov/research/publications/publications.htm?SEQ_NO_115=313160

1: J Infect Dis 1980 Aug;142(2):205-8

Oral transmission of kuru, Creutzfeldt-Jakob disease, and scrapie to nonhuman primates.

Gibbs CJ Jr, Amyx HL, Bacote A, Masters CL, Gajdusek DC.

Kuru and Creutzfeldt-Jakob disease of humans and scrapie disease of sheep and goats were transmitted to squirrel monkeys (Saimiri sciureus) that were exposed to the infectious agents only by their nonforced consumption of known infectious tissues. The asymptomatic incubation period in the one monkey exposed to the virus of kuru was 36 months; that in the two monkeys exposed to the virus of Creutzfeldt-Jakob disease was 23 and 27 months, respectively; and that in the two monkeys exposed to the virus of scrapie was 25 and 32 months, respectively. Careful physical examination of the buccal cavities of all of the monkeys failed to reveal signs or oral lesions. One additional monkey similarly exposed to kuru has remained asymptomatic during the 39 months that it has been under observation.

snip...

The successful transmission of kuru, Creutzfeldt-Jakob disease, and scrapie by natural feeding to squirrel monkeys that we have reported provides further grounds for concern that scrapie-infected meat may occasionally give rise in humans to Creutzfeldt-Jakob disease.

PMID: 6997404


Recently the question has again been brought up as to whether scrapie is transmissible to man. This has followed reports that the disease has been transmitted to primates. One particularly lurid speculation (Gajdusek 1977) conjectures that the agents of scrapie, kuru, Creutzfeldt-Jakob disease and transmissible encephalopathy of mink are varieties of a single "virus". The U.S. Department of Agriculture concluded that it could "no longer justify or permit scrapie-blood line and scrapie-exposed sheep and goats to be processed for human or animal food at slaughter or rendering plants" (ARC 84/77)" The problem is emphasised by the finding that some strains of scrapie produce lesions identical to the once which characterise the human dementias"

Whether true or not. the hypothesis that these agents might be transmissible to man raises two considerations. First, the safety of laboratory personnel requires prompt attention. Second, action such as the "scorched meat" policy of USDA makes the solution of the acrapie problem urgent if the sheep industry is not to suffer grievously.

snip...

76/10.12/4.6


Nature. 1972 Mar 10;236(5341):73-4.

Transmission of scrapie to the cynomolgus monkey (Macaca fascicularis).

Gibbs CJ Jr, Gajdusek DC.

Nature 236, 73 - 74 (10 March 1972); doi:10.1038/236073a0

Transmission of Scrapie to the Cynomolgus Monkey (Macaca fascicularis)

C. J. GIBBS jun. & D. C. GAJDUSEK

National Institute of Neurological Diseases and Stroke, National Institutes of Health, Bethesda, Maryland

SCRAPIE has been transmitted to the cynomolgus, or crab-eating, monkey (Macaca fascicularis) with an incubation period of more than 5 yr from the time of intracerebral inoculation of scrapie-infected mouse brain. The animal developed a chronic central nervous system degeneration, with ataxia, tremor and myoclonus with associated severe scrapie-like pathology of intensive astroglial hypertrophy and proliferation, neuronal vacuolation and status spongiosus of grey matter. The strain of scrapie virus used was the eighth passage in Swiss mice (NIH) of a Compton strain of scrapie obtained as ninth intracerebral passage of the agent in goat brain, from Dr R. L. Chandler (ARC, Compton, Berkshire).


Sunday, January 10, 2021 
APHIS Concurrence With OIE Risk Designation for Bovine Spongiform Encephalopathy [Docket No. APHIS-2018-0087] Singeltary Submission June 17, 2019

APHIS Concurrence With OIE Risk Designation for Bovine Spongiform Encephalopathy [Docket No. APHIS-2018-0087] Singeltary Submission

Greetings APHIS et al, 

I would kindly like to comment on APHIS Concurrence With OIE Risk Designation for Bovine Spongiform Encephalopathy [Docket No. APHIS-2018-0087], and my comments are as follows, with the latest peer review and transmission studies as references of evidence.

THE OIE/USDA BSE Minimal Risk Region MRR is nothing more than free pass to import and export the Transmissible Spongiform Encephalopathy TSE Prion disease. December 2003, when the USDA et al lost it's supposedly 'GOLD CARD' ie BSE FREE STATUS (that was based on nothing more than not looking and not finding BSE), once the USA lost it's gold card BSE Free status, the USDA OIE et al worked hard and fast to change the BSE Geographical Risk Statuses i.e. the BSE GBR's, and replaced it with the BSE MRR policy, the legal tool to trade mad cow type disease TSE Prion Globally. The USA is doing just what the UK did, when they shipped mad cow disease around the world, except with the BSE MRR policy, it's now legal. 

Also, the whole concept of the BSE MRR policy is based on a false pretense, that atypical BSE is not transmissible, and that only typical c-BSE is transmissible via feed. This notion that atypical BSE TSE Prion is an old age cow disease that is not infectious is absolutely false, there is NO science to show this, and on the contrary, we now know that atypical BSE will transmit by ORAL ROUTES, but even much more concerning now, recent science has shown that Chronic Wasting Disease CWD TSE Prion in deer and elk which is rampant with no stopping is sight in the USA, and Scrapie TSE Prion in sheep and goat, will transmit to PIGS by oral routes, this is our worst nightmare, showing even more risk factors for the USA FDA PART 589 TSE PRION FEED ban. 

The FDA PART 589 TSE PRION FEED ban has failed terribly bad, and is still failing, since August 1997. there is tonnage and tonnage of banned potential mad cow feed that went into commerce, and still is, with one decade, 10 YEARS, post August 1997 FDA PART 589 TSE PRION FEED ban, 2007, with 10,000,000 POUNDS, with REASON, Products manufactured from bulk feed containing blood meal that was cross contaminated with prohibited meat and bone meal and the labeling did not bear cautionary BSE statement. you can see all these feed ban warning letters and tonnage of mad cow feed in commerce, year after year, that is not accessible on the internet anymore like it use to be, you can see history of the FDA failure August 1997 FDA PART 589 TSE PRION FEED ban here, but remember this, we have a new outbreak of TSE Prion disease in a new livestock species, the camel, and this too is very worrisome.

WITH the OIE and the USDA et al weakening the global TSE prion surveillance, by not classifying the atypical Scrapie as TSE Prion disease, and the notion that they want to do the same thing with typical scrapie and atypical BSE, it's just not scientific.

WE MUST abolish the BSE MRR policy, go back to the BSE GBR risk assessments by country, and enhance them to include all strains of TSE Prion disease in all species. With Chronic Wasting CWD TSE Prion disease spreading in Europe, now including, Norway, Finland, Sweden, also in Korea, Canada and the USA, and the TSE Prion in Camels, the fact the the USA is feeding potentially CWD, Scrapie, BSE, typical and atypical, to other animals, and shipping both this feed and or live animals or even grains around the globe, potentially exposed or infected with the TSE Prion. this APHIS Concurrence With OIE Risk Designation for Bovine Spongiform Encephalopathy [Docket No. APHIS-2018-0087], under it's present definition, does NOT show the true risk of the TSE Prion in any country. as i said, it's nothing more than a legal tool to trade the TSE Prion around the globe, nothing but ink on paper.

AS long as the BSE MRR policy stays in effect, TSE Prion disease will continued to be bought and sold as food for both humans and animals around the globe, and the future ramifications from friendly fire there from, i.e. iatrogenic exposure and transmission there from from all of the above, should not be underestimated. ... 






Control of Chronic Wasting Disease OMB Control Number: 0579-0189 APHIS-2021-0004 Singeltary Submission



Docket No. APHIS-2018-0011 Chronic Wasting Disease Herd Certification


FRIDAY, DECEMBER 24, 2021 

Creutzfeldt Jakob Disease CJD TSE Prion Update December 25, 2021


Friday, March 11, 2022 

Prevalence of Surgical Procedures at Symptomatic Onset of Prion Disease


Terry S. Singeltary Sr.

posted by Terry S. Singeltary Sr. at 4:54 PM