Abstract
Autopsy rates are declining, while major discrepancies between autopsies and clinical diagnoses remain. Still, little is known about the impact of suspected underlying diseases, for example, a diagnosis of cancer, on the autopsy rate. The aim of this study was to investigate the relation between the clinical cause of death, a history of cancer, and the medical autopsy rate using data from the Netherlands Cohort Study on Diet and Cancer (NLCS), a large prospective cohort study with a long follow-up. The NLCS is a prospective study initiated in 1986 and includes 120,852 persons (58,279 males and 62,573 females), 55–69 years of age at the time of enrollment. The NLCS was linked with the Dutch Nationwide Pathology Databank (PALGA), the Dutch Population Register (GBA), the Netherlands Cancer Registry, and the causes of death registry (Statistics Netherlands). If applicable, the 95% confidence intervals were calculated. During the follow-up of the NLCS, 59,760 deaths were recorded by linkage with the GBA from 1991 until 2009. Of these, a medical autopsy was performed on 3736 deceased according to linkage with PALGA, resulting in an overall autopsy rate of 6.3%. Major variations in the autopsy rate were observed according to the cause of death. The autopsy rate increased according to the number of contributing causes of death. Lastly, a diagnosis of cancer affected the autopsy rate. The clinical cause of death and a history of cancer both influenced the medical autopsy rate in a large national cohort. The insight this study provides may help clinicians and pathologists counteracting the further downfall of the medical autopsy.
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Introduction
Medical autopsy stood at the basis of many important advances in medicine and health care [1, 2]. Nonetheless, over the last decades, a steady worldwide decline of autopsies has been observed [3-6]. Several explanations for this decline have been proposed, such as the attitude of the public, clinicians, and pathologists [7-9], lack of education in medical curricula [10], a shift in care for older or sicker people from the hospital towards long-term facilities [11], the financial aspects [12], and advances in minimally invasive alternatives [13-17]. A recent Dutch study suggests that a key aspect for not requesting an autopsy is the assumption that the cause of death is already known [18]. However, major discrepancies between autopsies and clinical diagnoses remain, even in this modern era [19-25]. Of interest, throughout the year 2020, autopsies have seen a small revival due to COVID-19 [26, 27]. Still, little is known about the impact of clinically suspected underlying diseases, e.g., a cancer diagnosis, on the autopsy rate.
The aim of this study was to investigate the relation of the clinical cause of death and a history of cancer to the autopsy rate, using data from the Netherlands Cohort Study on Diet and Cancer (NLCS). The NLCS is a large prospective cohort study with a long follow-up that has been linked to multiple population and health registries, among them nationwide data from Statistics Netherlands (CBS) and the Dutch Nationwide Pathology Databank (PALGA) [28].
Method
The NLCS was initiated in 1986 and has been described in detail elsewhere [29]. In brief, this prospective study encompasses 120,852 persons (58,279 males and 62,573 females), 55–69 years of age at the time of enrollment, living in 204 municipalities located throughout the Netherlands. Participants of the study consented by completing and returning the questionnaire.
The vital status was obtained by record linkage with the Central Bureau of Genealogy (CBG) and the automated municipal population registries (GBA), which record information of all inhabitants in the Netherlands, including death, birth, and migration. Information regarding vital status was available for 99.7% of the cohort on the 31st of December 2014.
The deceased participants of the NLCS were followed up for the performance of a medical autopsy by record linkage with the PALGA database using a linkage protocol described by van den Brandt et al. [30]. In the PALGA, database autopsies are coded and are therefore clearly distinguishable from other pathology reports. Although the autopsy conclusions were available, these were not used for this study. The autopsy rate was calculated as the number of autopsies divided by the number of deaths.
The cause of death (COD) per individual was established by record linkage with the cause of death registry maintained by Statistics Netherlands. For this analysis, data was used for the period 1991–2009 because PALGA had nationwide coverage since 1991 [28], and the linkage to the cause of death registry was completed until the 31st of December 2009 at the moment of analysis. Statistics Netherlands is able to request an autopsy report to adjust the COD as stated on the death certificate; however, this is only done in a limited number of cases. Therefore, we can assume that the data consists mostly of the suspected COD as determined by the physician, with little to no adjustments due to the results of the postmortem, i.e., the clinical COD.
The underlying COD was grouped according to the BELDO list [31]. The BELDO list is a shortlist that aims to provide a quick overview of the most relevant (i.e., common) COD in the Netherlands [32]. The list was created by the CBS in 1993, was based on the International Classification of Diseases (ICD), and has been the basis for the European Shortlist, as created by Eurostat in August 1998. For an overview of the ICD-9 and ICD-10 codes of the BELDO list, see Table 2. The two groups of COD with the highest and the lowest autopsy rates were further investigated by examining the individual COD within these groups.
Lastly, an occurrence of cancer until the 31st of December 2009 was identified by linkage with the Netherlands Cancer Registry and PALGA. The most recent record of an invasive cancer, non-melanoma skin cancer excluded, was selected and the time between the date of cancer incidence and date of death was calculated. Categories were created as follows: 0–1 days; 2–31 days; 32–183 days; 184–365 days; 1– < 2 years; 2– < 3 years; 3– < 4 years; 4– < 5 years; 5– < 10 years; 10– < 15 years; 15– < 20 years, and 20 + years. As age has an important influence on the autopsy [6], the expected number of autopsies in the group with a diagnosis of cancer was calculated using the autopsy rate per 5-year age category in the group without a diagnosis of cancer. In other words, the expected number of autopsies was corrected for age and sex. Next, the observed/expected (O/E) ratio was calculated with 95% confidence intervals.
The autopsy rate was also calculated for each individual COD according to the BELDO list, the time of death in relation to a diagnosis of cancer, and the number of different COD per case. Next, an independent sample t-test was conducted to compare the number of COD in deceased with and without an autopsy.
Results
At the time of inclusion in this study (January 1st 1991), 114,401 of the 120,852 NLCS participants were still alive. The demographics, number of deaths, and autopsies in the NLCS are shown in Table 1. During the follow-up of the NLCS, 59,760 deaths were recorded by linkage with CBG and GBA from 1991 until 2009. Of these, an autopsy was performed on 3736 deceased according to linkage with PALGA, resulting in an overall autopsy rate of 6.3%. The autopsy rate varies according to age at death and sex.
The number and percentage of performed autopsies per underlying COD, as classified by the BELDO list, are shown in Table 2. The autopsy rate varies considerably among the grouped CODs. Of 181 (0,3%) included participants, the cause of death was not known, and the CBS was unable to apply a code. These cases mostly included a death abroad or administrative errors. In 16 (8.8%) of these, an autopsy was performed. In 1764 (3%), the cause of death was unclear, hence it was specified as “symptoms, signs, abnormal findings, ill-defined causes.” In 89 (5%) of these, an autopsy was performed. To our knowledge, the CBS only occasionally contacts clinicians in order to request the autopsy information for the purpose of a correct cause of death.
The highest autopsy rate was observed when the death certificate showed a COD related to the digestive system (16.9%), followed by infectious and parasitic diseases (14.3%). Table 3 shows the most common individual COD within the groups with the highest and the lowest autopsy rates. The diseases of the digestive system consisted of many different large subgroups with an autopsy rate of > 10%, while infectious and parasitic diseases consisted of a large subgroup ‘other sepsis’ (49.0%) with an autopsy rate of 18.8%.
Next, the least autopsies were performed in mental and behavioral diseases (0.8%) and diseases of the nervous system and the sense organs (4.0%). By far, the largest subgroup within the mental and behavioral diseases concerns the “unspecified dementia” (83.6%) followed by “vascular dementia” (13.3%), with both having an autopsy rate of 0.6%. Diseases of the nervous system and the sense organs mostly concerned “Parkinson’s disease” (38.7%) and “Alzheimer’s disease” (24.2%) with autopsy rates of 2.7% and 0.5%, respectively.
As shown in Table 4, the autopsy rate increased with an increasing number of contributing COD per deceased person. The autopsy rate for a deceased person with one declared COD was 5.2%. In contrast, the autopsy rate for a COD with three contributing causes of death was 8.0%. The independent sample t-test to compare the number of CODs in deceased with (1.72) and without (1.88) autopsies showed p < 0.001.
The autopsy rate after a clinical diagnosis of cancer is shown in Table 5. The autopsy rate in deceased without a clinical diagnosis of cancer was 4.4%. The overall autopsy rate for deceased with a previous clinical diagnosis of cancer was 6.2%. A higher or lower O/E ratio, respectively, signifies a higher or lower autopsy rate than expected, based on the autopsy rates per age category in deceased without a diagnosis of cancer. Incidental findings during the autopsy could not be excluded in the “0–1 days” group, which shows an autopsy rate of 78.0%. These included cancer of the lung, prostate, kidney, pancreas, large intestines, and lymphatic malignancies such as acute lymphocytic leukemia, non-Hodgkin, and Hodgkin lymphoma. When we excluded the first 0–1 days, the autopsy rate was 5.2%. There was a higher autopsy rate than expected in the first month (2–31 days) after a diagnosis of cancer, a slightly lower autopsy rate than expected in the months and years thereafter, and a stabilization after approximately 15 years. Most deaths occurred within 1 year after a diagnosis of cancer (n = 9363), mostly within the “32–183 days” category (48%).
Discussion
Our study investigates the relation between the clinical cause of death, a history of cancer, and the autopsy rate by linking the NLCS to nationwide databases: the cancer registry, the Dutch Nationwide Pathology Databank (PALGA), the population registry, and the cause of death registry. The cause of death registry uses death certificates that are completed by physicians, usually within a few hours after a patient dies and before an autopsy is performed. To our knowledge, this linkage between clinical COD and the autopsy rate has not been investigated before. As in most European countries, permission for a clinical autopsy needs to be consented to by the relatives. In the Netherlands, this is done orally. This presumably results in more reluctance compared to countries in which no consent is needed, or autopsies are obligatory, especially in the older age categories. Consequently, in the Netherlands, the autopsy rate is among the lowest in Europe [6]. In a national study encompassing all clinical autopsies in the Netherlands, the autopsy rate in the age category 60–79 declined from just below 10% to approximately 3.9% from 1991 to 2015. In addition, the autopsy rate varied between different age categories, i.e., an average autopsy rate of 8.06% in the age category 60–64 years and 1.12% in 90–94 years. Lastly, a difference in autopsy rate according to sex could be explained by the age difference at the time of death. Our study shows a similar decreasing autopsy rate with older age, as shown in Table 1. More than half of all participants died from 1991 to 2009, mostly between the ages of 65 and 84 years. Contrarily, in all age categories, the autopsy rate was higher in males.
The results show a varying autopsy rate with different CODs, as shown in Table 2. Some considerations can be made when looking at the ICD codes that constitute the BELDO list, as shown in Tables 2 and 3. The autopsy rate in different CODs is derived from the NLCS, which is a population aged 55–70 at baseline in 1986, with a follow-up of 23 years. Although most deaths in the Netherlands occur in these age groups, these findings cannot be extrapolated to all patients as the COD distribution varies with age.
The most important consideration for relatives to give permission for an autopsy is the wish to learn about the cause of death [18]. The highest autopsy rate was observed in COD related to the digestive system (16.9%), followed by infectious and parasitic diseases (14.3%). Infectious and parasitic diseases can develop quite fast and are unpredictable, but as a CODs, they are rather rare in the Netherlands. This might explain the relatively high autopsy rate. One would expect this number to have increased even more in the face of the COVID-19 pandemic, but this is outside the time frame of this study. One could argue diseases of the digestive system may cause vague symptoms, which might lead to an unexpected and/or unexplained demise, therefore increasing the “need to know” of relatives and physicians.
Next, the autopsy rate was lowest in mental and behavioral diseases (0.8%) and diseases of the nervous system and the sense organs (4.0%). Of all the deaths in the “mental and behavioral diseases” group, 83.6% consisted of “unspecified dementia,” which was rated number 7 in the list of most common causes of death in 2000 in the Netherlands [32]. As patients with dementia are more prone to demise at home or in a nursing home, this might lead to a difference in autopsy rate, as shown by Lindstrom [3]. In addition, due to the long process of the disease, next of kin and physicians might be less inclined to refer to an autopsy [18]. A similar explanation is applicable to Alzheimer’s and Parkinson’s diseases in the group “diseases of the nervous system and sense organs.” An important reason for not requesting or permitting an autopsy is the assumption that the cause of death is already known [18]. This might be a feasible explanation for the low autopsy rate in deaths due to dementia, Parkinson’s disease, and Alzheimer’s disease. For the sake of completeness, there was one death due to an unspecified perinatal disease of the digestive tract, without an autopsy, which could either be a coding error or a very late death because of a congenital abnormality.
Our results show that the autopsy rate was positively correlated with the number of contributing causes of death (Table 4). This suggests physicians are more likely to request an autopsy when confronted with complex cases. However, due to technical and/or legal limits, death certificates are mostly completed before the conclusions of a postmortem become available. Despite improvements in clinical healthcare and technical advances in the last decades, a significant amount of major and minor discrepancies between clinical diagnoses and autopsy findings still remain [7, 20-22, 24, 33]. Major discrepancies are findings associated with the COD, where prior knowledge ante mortem might have changed patient management and survival in some cases. A study in the Netherlands showed major discrepancies in 16% of the autopsies in 2012/2013 [19]. Thus, autopsies continue to provide invaluable information for medical education and quality assurance [1]. Autopsies in particular have also been used as a measure for the accuracy of death certificates in general populations [34, 35] and in selected groups of diseases [36]. Therefore, some authors suggested that death certificates should be completed or amended utilizing data gained during autopsy [37]. Death certificates are the main source for mortality statistics and, as an indicator, contribute greatly to detecting trends in (inter)national healthcare [38]. As physicians are required to complete the death certificate, they play an important role in mortality statistics, and therefore indirectly, in the distribution of resources in healthcare and research.
In our study, the autopsy rate was affected by a diagnosis of cancer, most dramatically in deaths within 31 days after a diagnosis of cancer (Table 5). This increase in the first month could be explained by a sudden unset and/or rapid increase of the cancer, which may lead to unanswered questions for physicians and relatives. In the months and years thereafter, the cancer and possible cause of death would be known, which could lead to a decreased interest in autopsies, up to the stabilization after some 15 years.
The effect of completing death certificates without autopsy results, in regard to the incidence of cancer, is inconsistent. A study from 1997 conducted in Sweden suggested that the incomplete postmortem information due to the decline of autopsies was associated with a difference in the registered incidence of cancer [3]. However, in another study published in 2015 in Switzerland [39], the total registered incidence of cancers was not affected by the lower autopsy rate, perhaps due to advances in modern diagnostic tools as suggested by the authors. Another explanation for the contrasting results of both studies might be methodological and structural differences in the organization of the cancer registries within the two healthcare systems. In our study, a diagnosis on days 0–1 most likely means the cancer was detected as an incidental finding, i.e., during the autopsy, and was thereafter recorded in the cancer registry. Alternatively, the cancer was identified during a medical procedure such as surgery, after which the patient died, and the diagnosis was confirmed during an autopsy. In other words, the cancer was presumably undiagnosed before passing away in most of these cases. This probably explains the significantly higher autopsy rate of 78.0% on days 0–1. As there are only 269 autopsies with a diagnosis of cancer on day 0–1 in a study group with almost 25,000 patients with cancer, a possible effect of a decreasing autopsy rate on the cancer incidence is limited. Blokker et al. [40] speculated that the lower autopsy rate in older patients might be correlated to an increased number of deaths due to cancer. This differs from the findings presented here, as our average autopsy rate in cancer patients was slightly higher than in patients without cancer, even after excluding the “0–1 days” group. Our results suggest that the lower autopsy rate in older patients is more likely due to death in cases of dementia, as discussed above.
In our study, the linkage with excerpts from the PALGA-database was used to investigate whether an autopsy was performed. Not being able to see the full autopsy report in PALGA is therefore a limitation. Access to this data, perhaps in comparison with the cause of death registry by the CBS, may provide additional interesting insights.
The relevance of autopsies has been described in numerous publications over the years. Although major discrepancies between autopsies and clinical diagnoses remain [19,20,21,22,23,24,25], a steady worldwide decline of autopsies has been observed [3,4,5,6]. Therefore, it is the opinion of the authors that medical healthcare in general, as well as individuals, would benefit from an increase in postmortem investigations, among which autopsies. This increase can only be effectuated in close collaboration with clinicians and should be a solution for a problem, not the mere goal.
Conclusion
This study shows the relation between the clinical cause of death, a history of cancer, and the medical autopsy rate in a large national cohort. There were major variations in the autopsy rate in relation to the clinically reported cause of death. The autopsy rate was positively correlated with the number of contributing causes of death, suggesting a higher interest in autopsies in complex medical cases. Lastly, the presence of cancer only showed an increased autopsy rate in the first year after diagnosis. The insight this study provides may help clinicians and pathologists to understand the decreasing autopsy rate and intervene in the further downfall of the medical autopsy.
References
Zampieri F, Rizzo S, Thiene G, Basso C (2015) The clinico-pathological conference, based upon Giovanni Battista Morgagni’s legacy, remains of fundamental importance even in the era of the vanishing autopsy. Virchows Arch 467(3):249–254
Burton EC (2002) The autopsy: a professional responsibility in assuring quality of care. Am J Med Qual 17(2):56–60
Lindstrom P, Janzon L, Sternby NH (1997) Declining autopsy rate in Sweden: a study of causes and consequences in Malmo. Sweden J Intern Med 242(2):157–165
Loughrey MB, McCluggage WG, Toner PG (2000) The declining autopsy rate and clinicians’ attitudes. Ulster Med J 69(2):83–89
Turnbull A, Osborn M, Nicholas N (2015) Hospital autopsy: endangered or extinct? J Clin Pathol 68(8):601–604
Latten BGH, Overbeek LIH, Kubat B, ZurHausen A, Schouten LJ (2019) A quarter century of decline of autopsies in the Netherlands. Eur J Epidemiol 34(12):1171–1174
Burton JL, Underwood J (2007) Clinical, educational, and epidemiological value of autopsy. Lancet 369(9571):1471–1480
Stempsey WE (2016) The Penetrating gaze and the decline of the autopsy. AMA J Ethics 18(8):833–838
Burton EC, Phillips RS, Covinsky KE, Sands LP, Goldman L, Dawson NV et al (2004) The relation of autopsy rate to physicians’ beliefs and recommendations regarding autopsy. Am J Med 117(4):255–261
van den Tweel JG, Wittekind C (2016) The medical autopsy as quality assurance tool in clinical medicine: dreams and realities. Virchows Arch 468(1):75–81
Gaensbacher S, Waldhoer T, Berzlanovich A (2012) The slow death of autopsies: a retrospective analysis of the autopsy prevalence rate in Austria from 1990 to 2009. Eur J Epidemiol 27(7):577–580
Adviesrapport Postmortem diagnostiek (2020) (Nederlandse Vereniging voor Pathologie)
Roberts IS, Benamore RE, Benbow EW, Lee SH, Harris JN, Jackson A et al (2012) Post-mortem imaging as an alternative to autopsy in the diagnosis of adult deaths: a validation study. Lancet 379(9811):136–142
Blokker BM, Wagensveld IM, Weustink AC, Oosterhuis JW, Hunink MG (2016) Non-invasive or minimally invasive autopsy compared to conventional autopsy of suspected natural deaths in adults: a systematic review. Eur Radiol 26(4):1159–1179
Latten BGH, Bakers FCH, Hofman PAM, ZurHausen A, Kubat B (2019) The needle in the haystack: histology of post-mortem computed tomography guided biopsies versus autopsy derived tissue. Forensic Sci Int 302:109882
Mentink MG, Bakers FCH, Mihl C, Lahaye MJ, Rennenberg R, Latten BGH, et al (2020) Introduction of postmortem CT increases the postmortem examination rate without negatively impacting the rate of traditional autopsy in daily practice: an implementation study. J Clin Pathol
Ampanozi G, Halbheer D, Ebert LC, Thali MJ, Held U (2020) Postmortem imaging findings and cause of death determination compared with autopsy: a systematic review of diagnostic test accuracy and meta-analysis. Int J Legal Med 134(1):321–337
Blokker BM, Weustink AC, Hunink MG, Oosterhuis JW (2016) Autopsy of adult patients deceased in an academic hospital: considerations of doctors and next-of-kin in the consent process. PLoS ONE 11(10):e0163811
Kuijpers CC, Fronczek J, van de Goot FR, Niessen HW, van Diest PJ, Jiwa M (2014) The value of autopsies in the era of high-tech medicine: discrepant findings persist. J Clin Pathol 67(6):512–519
Wittschieber D, Klauschen F, Kimmritz AC, von Winterfeld M, Kamphues C, Scholman HJ et al (2012) Who is at risk for diagnostic discrepancies? Comparison of pre- and postmortal diagnoses in 1800 patients of 3 medical decades in East and West Berlin. PLoS ONE 7(5):e37460
Schwanda-Burger S, Moch H, Muntwyler J, Salomon F (2012) Diagnostic errors in the new millennium: a follow-up autopsy study. Mod Pathol 25(6):777–783
Shojania KG, Burton EC, McDonald KM, Goldman L (2003) Changes in rates of autopsy-detected diagnostic errors over time: a systematic review. JAMA 289(21):2849–2856
Battle RM, Pathak D, Humble CG, Key CR, Vanatta PR, Hill RB et al (1987) Factors influencing discrepancies between premortem and postmortem diagnoses. JAMA 258(3):339–344
Goldman L, Sayson R, Robbins S, Cohn LH, Bettmann M, Weisberg M (1983) The value of the autopsy in three medical eras. N Engl J Med 308(17):1000–1005
Goldman L (2018) Autopsy 2018: still necessary, even if occasionally not sufficient. Circulation 137(25):2686–8
Carsana L, Sonzogni A, Nasr A, Rossi RS, Pellegrinelli A, Zerbi P et al (2020) Pulmonary post-mortem findings in a series of COVID-19 cases from northern Italy: a two-centre descriptive study. Lancet Infect Dis 20(10):1135–1140
Maiese A, Manetti AC, La Russa R, Di Paolo M, Turillazzi E, Frati P, et al (2020) Autopsy findings in COVID-19-related deaths: a literature review. Forensic Sci Med Pathol
Casparie M, Tiebosch AT, Burger G, Blauwgeers H, van de Pol A, van Krieken JH et al (2007) Pathology databanking and biobanking in The Netherlands, a central role for PALGA, the nationwide histopathology and cytopathology data network and archive. Cell Oncol 29(1):19–24
van den Brandt PA, Goldbohm RA, van’t Veer P, Volovics A, Hermus RJ, Sturmans F (1990) A large-scale prospective cohort study on diet and cancer in The Netherlands. J Clin Epidemiol 43(3):285–95
Van den Brandt PA, Schouten LJ, Goldbohm RA, Dorant E, Hunen PM (1990) Development of a record linkage protocol for use in the Dutch Cancer Registry for Epidemiological Research. Int J Epidemiol 19(3):553–558
Statistics Netherlands (1993) Alterations in the presentation of demographic data and cause of death. Maandbericht Gezondheidsstatistiek. 1993(juli):34–5
Verweij G (2002) A closer look at the list of important causes of death [in Dutch]. Maandstatistiek van de bevolking. Jaargang 50(maart 2002)
Winters B, Custer J, Galvagno SM Jr, Colantuoni E, Kapoor SG, Lee H et al (2012) Diagnostic errors in the intensive care unit: a systematic review of autopsy studies. BMJ Qual Saf 21(11):894–902
Nash I (1986) The autopsy as a measure of accuracy of the death certificate. N Engl J Med 314(19):1259
McKelvie PA (1993) Medical certification of causes of death in an Australian metropolitan hospital. Comparison with autopsy findings and a critical review. Med J Aust 158(12):816-8–20-1
Tavora F, Crowder C, Kutys R, Burke A (2008) Discrepancies in initial death certificate diagnoses in sudden unexpected out-of-hospital deaths: the role of cardiovascular autopsy. Cardiovasc Pathol 17(3):178–182
Smith Sehdev AE, Hutchins GM (2001) Problems with proper completion and accuracy of the cause-of-death statement. Arch Intern Med 161(2):277–284
Hoel DG, Ron E, Carter R, Mabuchi K (1993) Influence of death certificate errors on cancer mortality trends. J Natl Cancer Inst 85(13):1063–1068
Bieri U, Moch H, Dehler S, Korol D, Rohrmann S (2015) Changes in autopsy rates among cancer patients and their impact on cancer statistics from a public health point of view: a longitudinal study from 1980 to 2010 with data from Cancer Registry Zurich. Virchows Arch 466(6):637–643
Blokker BM, Weustink AC, Hunink MGM, Oosterhuis JW (2017) Autopsy rates in the Netherlands: 35 years of decline. PLoS ONE 12(6):e0178200
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LS and BL performed study concept and design. LS analyzed the data, partly according to the protocol created by PB. BL drafted the manuscript. BL, LS, BK, PB, and AH reviewed the manuscript.
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Approval for the NLCS was granted by institutional review boards from Maastricht University in 1985, and the Netherlands Organization for Applied Scientific Research in 1986. All cohort members consented to participate in the study by completing and returning the self-administered questionnaire. As this study involves deceased it is not subject to the Medical Research Involving Human Subjects Act (WMO).
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Latten, B.G.H., Kubat, B., van den Brandt, P.A. et al. Cause of death and the autopsy rate in an elderly population. Virchows Arch 483, 865–872 (2023). https://doi.org/10.1007/s00428-023-03571-0
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DOI: https://doi.org/10.1007/s00428-023-03571-0