Premenstrual Syndrome Diagnosis: A Comparative Study between the Daily Record of Severity of Problems (DRSP) and the Premenstrual Symptoms Screening Tool (PSST)

Henz, Aline; Ferreira, Charles Francisco; Oderich, Carolina Leão; Gallon, Carin Weirich; Castro, Juliana Rintondale Sodré de; Conzatti, Maiara; Fleck, Marcelo Pio de Almeida; Wender, Maria Celeste Osório

doi:10.1055/s-0037-1608672

Abstract

Objective

To validate the premenstrual symptoms screening tool (PSST) in relation to the daily record of severity of problems (DRSP) for premenstrual syndrome (PMS) and premenstrual dysphoric disorder (PMDD) diagnoses.

Methods

A cross-sectional study with 127 women (20 45 years) with PMS complaints. The women were evaluated in terms of weight, height and body mass index (BMI). After using the primary care evaluation of mental disorders (PRIME-MD) questionnaire to exclude the diagnosis of depression, the PSST was completed and the women were instructed to fill out the DRSP for two consecutive menstrual cycles. The agreement between the two questionnaires was assessed by the Kappa (k) and the prevalence-adjusted, bias-adjusted kappa (PABAK) values.

Results

Two-hundred and eighty-two women met the eligibility criteria and answered the PSST. The DRSP was completed for two cycles by 127 women. The percentages of women with PMS and PMDD diagnoses by the DRSP were 74.8% and 3.9% respectively; by PSST, the percentages were41.7% and 34.6% respectively. The number of patients considered "normal" (with symptoms below the threshold for the diagnosis of PMS) was similar in both questionnaires. There was no agreement (Kappa = 0.12) in the results of PMS/ PMDD diagnosis (the PABAK coefficient confirmed this result = 0.39). The PSST had a high sensitivity (79%) and a low specificity (33.3%) for PMS/PMDD diagnosis.

Conclusion

The PSST should be considered a diagnostic screening tool. Positive PMS/PMDD cases by PSST should be further evaluated by DRSP to confirm the diagnosis.

Keywords:
diagnosis; questionnaire; signs and symptoms; premenstrual syndrome; premenstrual dysphoric disorder

Resumo

Objetivo

Validar o instrumento de rastreamento de sintomas pré-menstruais (PSST) em relação ao relato diário da gravidade dos problemas (DRSP) para o diagnóstico de síndrome pré-menstrual (SPM) e de transtorno disfórico pré-menstrual (TDPM).

Métodos

Um estudo transversal com 127 mulheres entre 20 e 45 anos com queixas de SPM. As mulheres foram avaliadas quanto ao peso, à altura e ao índice de massa corporal (IMC). Depois de excluir o diagnóstico de depressão pelo questionário de avaliação de distúrbios mentais para atenção primária (PRIME-MD), o PSST foi respondido e as mulheres receberam orientações sobre como preencher o DRSP por dois meses. A concordância entre os dois questionários foi conduzida através do índice de Kapa (k) e pelo PABAK.

Resultados

Duzentos e oitenta e duas mulheres com critérios elegíveis responderam ao PSST. O DRSP foi preenchido por dois ciclos por 127 mulheres. As porcentagens de mulheres com diagnósticos de SPM e de TDPM pelo DRSP foram de 74,8% e 3,9%, respectivamente; pelo PSST, as porcentagens foram de 41,7% e 34,6%, respectivamente. O número de pacientes consideradas "normais" (com sintomas abaixo do necessário para o diagnóstico de SPM) foi similar nos dois questionários. Análises demonstraram não haver concordância entre ambos os instrumentos para os resultados diagnósticos de SPM e TDPM (Kappa = 0,12, coeficiente de PABAK = 0,39). Para o diagnóstico de SPM/TDPM, o PSST apresentou uma alta sensibilidade (79%) e baixa especificidade (33,3%).

Conclusão

O PSST é considerado uma ferramenta de triagem. Conclui-se que casos positivos de SPM/TDPM pelo PSST devem ser melhor investigados pelo DRSP para confirmar o diagnóstico.

Palavras-Chave:
diagnóstico; questionário; sinais e sintomas; síndrome prémenstrual; transtorno disfórico prémenstrual

Introduction

Premenstrual syndrome (PMS) is defined as a recurring pattern of symptoms that occur during the premenstrual phase and decline soon after the start of menses.¹1 Nillni YI, Rohan KJ, Zvolensky MJ. The role of menstrual cycle phase and anxiety sensitivity in catastrophicmisinterpretation of physical symptoms during a CO(2) challenge. Arch Women Ment Health 2012;15(06):413-422 It is characterized by physical, affective, and behavioral symptoms that significantly impair the daily lives of women, including work and personal activities, during the luteal phase and spontaneously resolve within a few days of the onset of menstruation.²2 Ryu A, KimTH. Premenstrual syndrome: Amini review.Maturitas 2015;82(04):436-440

About 50–80% of women report that they experience at least some PMS symptoms during the premenstrual phase, and the condition occurs in approximately 30–40% of reproductive females that report symptoms of PMS, who end up requiring some type of treatment or better attention.¹1 Nillni YI, Rohan KJ, Zvolensky MJ. The role of menstrual cycle phase and anxiety sensitivity in catastrophicmisinterpretation of physical symptoms during a CO(2) challenge. Arch Women Ment Health 2012;15(06):413-422 ²2 Ryu A, KimTH. Premenstrual syndrome: Amini review.Maturitas 2015;82(04):436-440 ³3 Kessel B. Premenstrual syndrome. Advances in diagnosis and treatment. Obstet Gynecol Clin North Am 2000;27(03):625-639 ⁴4 Halbreich U, Borenstein J, Pearlstein T, Kahn LS. The prevalence, impairment, impact, andburdenofpremenstrualdysphoricdisorder (PMS/PMDD). Psychoneuroendocrinology 2003;28(Suppl 3):1-23 ⁵5 Rodrigues IC, Oliveira E. Prevalência e convivência demulheres com síndrome pré-menstrual. Arq Ciênc Saúde. 2006;13:146-152 ⁶6 Petta CA, Osis MJ, de Pádua KS, Bahamondes L, Makuch MY. Premenstrual syndrome as reported by Brazilian women. Int J Gynaecol Obstet 2010;108(01):40-43 ⁷7 Miller FC. Ten goals for the American College of Obstetricians and Gynecologists for the first decade of the next millennium. Obstet Gynecol 2000;95(01):1-5 ⁸8 Wittchen HU, Becker E, Lieb R, Krause P. Prevalence, incidence and stability of premenstrual dysphoric disorder in the community. Psychol Med 2002;32(01):119-132

Women with severe symptoms, including at least one disabling affective symptom, to the extent of causing marked functional impairment are classified as having premenstrual dysphoric disorder (PMDD). It is estimated that PMDD affects from 3–8% of menstruating women.⁹9 Heinemann LA, Minh TD, Filonenko A, Uhl-Hochgräber K. Explorative evaluation of the impact of severe premenstrual disorders on work absenteeism and productivity. Womens Health Issues 2010;20(01):58-65

The symptoms of PMS can be very similar to those of other diseases, such as depression and anxiety crisis, among others; therefore, an accurate prospective evaluation of the symptoms is required to make the diagnosis. The International Society for Premenstrual Disorders (ISPMD) recommends that the diagnosis is only confirmed after reviewing the data recorded for 2 consecutive menstrual cycles.¹⁰10 Nevatte T, O'Brien PM, Bäckström T, et al; Consensus Group of the International Society for Premenstrual Disorders. ISPMD consensus on the management of premenstrual disorders. ArchWomen Ment Health 2013;16(04):279-291

The use of structured questionnaires is established, and several validated diagnostic techniques are available. The most accepted and widely used system is the daily record of severity problems (DRSP), a prospective, self-administered questionnaire. To use the DRSP as a diagnostic tool for PMS, it is necessary that the patient fills it for at least two consecutive menstrual cycles. However, this requirement limits this practical applicability in the day-to-day care of patients with premenstrual symptoms.¹¹11 O'Brien PM, Bäckström T, Brown C, et al. Towards a consensus on diagnostic criteria,measurement and trial design of the premenstrual disorders: the ISPMD Montreal consensus. Arch Women Ment Health 2011;14(01):13-21 ¹²12 Endicott J, Nee J, HarrisonW. Daily Record of Severity of Problems (DRSP): reliability and validity. ArchWomen Ment Health 2006;9 (01):41-49 ¹³13 Borenstein JE, Dean BB, Yonkers KA, Endicott J. Using the daily record of severity of problems as a screening instrument for premenstrual syndrome.ObstetGynecol 2007;109(05):1068-1075

The premenstrual symptoms screening tool (PSST) is a retrospective questionnaire completed during clinical consultation with the patient. It is a screening tool used to identify women who suffer from severe PMS/PMDD.¹⁴14 Steiner M, Macdougall M, Brown E. The premenstrual symptoms screening tool (PSST) for clinicians. Arch Women Ment Health 2003;6(03):203-209 It is less time-consuming and more practical than two cycles of prospective charting. However, the retrospective assessment of symptoms has limited value and requires validation against an established prospective technique, such as the DRSP.¹¹11 O'Brien PM, Bäckström T, Brown C, et al. Towards a consensus on diagnostic criteria,measurement and trial design of the premenstrual disorders: the ISPMD Montreal consensus. Arch Women Ment Health 2011;14(01):13-21

Based on these considerations, the aim of this study was to validate the PSST in relation to the DRSP for the diagnosis of PMS and PMDD.

Methods

The selected women read and signed the informed consent, which was approved by the Committee of Ethics in Research of the institution (number 15–0087).

This was a cross-sectional study with participants recruited by local media (TV, radio or newspaper) announcements. The study was developed in a hospital in the state of Rio Grande do Sul, Brazil, during the period from August of 2014 to December of 2015.

The participants were women between 20 and 45 years old with PMS complaints and cyclical menses. The exclusion criteria were: menopause, use of any continuous hormonal contraception, use of antidepressants or depression diagnosis.

It was determined that in order to get a Kappa coefficient of at least 0.7, with 80% power, and a level of significance of 5%, the sample size should comprise at least 123 valid questionnaires. The women included were evaluated in terms of weight, height and body mass index (BMI), and they all answered the primary care evaluation of mental disorders (PRIME-MD) questionnaire (Module mood). In the cases of positive screening for depression, the diagnostic and statistical manual of mental disorders (DSM-V) questionnaire was applied to establish the diagnosis. The depressive women were excluded from the study and referred for psychiatric care. After the PSST (Supplemental Material 1) was completed by the women, the DRSP (Supplemental Material 2) was handed out to be filled out daily for two consecutive menstrual cycles.¹²12 Endicott J, Nee J, HarrisonW. Daily Record of Severity of Problems (DRSP): reliability and validity. ArchWomen Ment Health 2006;9 (01):41-49 ¹³13 Borenstein JE, Dean BB, Yonkers KA, Endicott J. Using the daily record of severity of problems as a screening instrument for premenstrual syndrome.ObstetGynecol 2007;109(05):1068-1075 ¹⁴14 Steiner M, Macdougall M, Brown E. The premenstrual symptoms screening tool (PSST) for clinicians. Arch Women Ment Health 2003;6(03):203-209 ¹⁵15 Spitzer RL, Kroenke K,Williams JB. Validation and utility of a selfreport version of PRIME-MD: the PHQ primary care study. Primary Care Evaluation of Mental Disorders. Patient Health Questionnaire. JAMA 1999;282(18):1737-1744 ¹⁶16 Fraguas R Jr, Henriques SG Jr, De Lucia MS, et al. The detection of depression in medical setting: a study with PRIME-MD. J Affect Disord 2006;91(01):11-17 ¹⁷17 American Psychiatric Association. Diagnostic and statistical manual of mental disorders: DSM-5. 5th ed.Washington, DC: American Psychiatric Publishing; 2013 ¹⁸18 Câmara RA, Köhler CA, Frey BN, Hyphantis TN, Carvalho AF. Validation of the Brazilian Portuguese version of the Premenstrual Symptoms Screening Tool (PSST) and association of PSST scores with health-related quality of life. Rev Bras Psiquiatr 2017;39(02):140-146

Statistical analysis was performed using the software SPSS, version 18.0 (SPSS Inc., Chicago, IL, USA). Continuous variables were expressed as mean ± standard deviation (SD) and categorical variables were expressed as absolute (n) and relative (n%) frequencies. The agreement between the two questionnaires was evaluated by calculating the Kappa (k) and the prevalence-adjusted, bias-adjusted kappa (PABAK) values. Kappa is an agreement measure beyond that agreement expected to occur by chance. The Kappa expected, according to Altman,¹⁹19 Altman DG. Practical statistics for medical research. London: Chapman & Hall/CRC; 1990 was 0.8— with a range of 0.643–0.893, with a 95% confidence interval (95%CI). Additionally, an interval-by-interval basis was calculated by the PABAK.²⁰20 Byrt T, Bishop J, Carlin JB. Bias, prevalence and kappa. J Clin Epidemiol 1993;46(05):423-429 The PABAK is a simple and flexible index, representing a method for calculating inter-rater reliability between two raters (for example, DRSP and PSST) using an ordinal rating scale of categories (such as, Normal, PMS and PMDD), suitable for nominal scales only. The PABAK value was calculated using the computer program for Epidemiologists WinPEPI, version 11.65 (for 2 × 2 categories tables), or the PABAK-OS calculator, available at singlecaseresearch.org (for table formats other than 2 × 2 categories). For all analyses, significance was set at 5%.

Results

Overall, 377 women signed up to participate in the study; however, only 282 (74%) of them were considered eligible due to category recruitment and thus, these women answered the PSST. The baseline characteristics of these women are shown in Table 1.

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Table 1
Sociodemographic characteristics of the women who completed the PSST and filled out the DRSP for 2 consecutive menstrual cycles

Of the eligible women, 135 (55%) did not fully complete all the two cycles of the daily questionnaire (DRSP). Only 127 (45%) women completed the study— including the 2 cycles of the DRSP. These women were considered to have fully participated in this study and represent the full analysis set (Fig. 1).

Fig. 1
The flowchart shows the selection process of the participants.

The Portuguese version of the DRSP was applied, and an initial exploration for the discriminant validity of this questionnaire was performed, proving the efficiency of its use for the diagnosis of PMS/PMDD. Confirming the diagnosis of PMS, the Supplemental Material 3 presents the medians of the DRSP scores for individual questions considering the luteal and follicular phases. The mean follicular phase scores were ≤ 30% of the luteal phase scores for at least 1 out of 3 different symptoms. Impressively, all of the DRSP items were significantly higher in the luteal phase when compared with the follicular phase, proving the sensitivity of this questionnaire for this purpose. These results support the validation of the DRSP instrument in Portuguese for the Brazilian population.

Fig. 2 shows that the diagnosis of PMS was higher with the DRSP, and the PMDD diagnosis was higher using the PSST. The percentage of PMS diagnosed by the DRSP was 74.8%, and 41.7% by the PSST; the percentage of PMDD by the DRSP was 3.9%, and 34.6% by the PSST. The number of patients that were considered “normal” was similar in both questionnaires.

Fig. 2
Comparative prevalence (percentage of total sample) of PMS/PMDD diagnosis between the PSST and the DRSP. Both instruments presented similar percentages for values falling within normal range. The PMS percentage was 74.8 by DRSP and 41.7 by PSST. The PMDD percentage was 3.9 by DRSP and 34.6 by PSST. Abbreviations: DRSP, daily record of severity problems; PMDD, premenstrual dysphoric disorder; PMS, premenstrual syndrome; PSST, premenstrual symptoms screening tool.

When we compare the diagnosis in both questionnaires, 70% of the women considered “normal” by PSST had a PMS diagnosis after the DRSP and 83% of the women with PMS diagnosis by PSST had the PMS diagnosis confirmed by the DRSP. Otherwise, only 6.8% of the PMDD diagnosis by the PSST had a PMDD diagnosis by the DRSP, and 68.2% of the PMDD diagnosis by the PSST had a PMS diagnosis by the DRSP (Fig. 3).

Fig. 3
Assessment of the PSST results according to DRSP diagnosis. Normal percentage by PSST (70%, light gray column in normal) would be classified as PMS by DRSP diagnosis. Premenstrual syndrome percentage by PSST (83%, light gray column in PMS) with confirmed PMS diagnosis by DRSP. Premenstrual dysphoric disorder percentage by PSST (6.8%, darker gray column in PMDD) with confirmed PMDD diagnosis by DRSP. Premenstrual dysphoric disorder percentage by PSST (68.2%, light gray column in PMDD) would be classified as PMS by DRSP diagnosis. Abbreviations: DRSP, daily record of severity problems; PMDD, premenstrual dysphoric disorder; PMS, premenstrual syndrome; PSST, premenstrual symptoms screening tool.

When considering all the frequencies in the diagnosis categories (Normal, PMS and PMDD) between the DRSP and PSST, an agreement between both instruments could not be observed, as illustrated by the value of the Kappa coefficient (k = 0.104, 95%CI [0.001–0.207], p= 0.039). Even when considering the adjusted prevalence through the PABAK coefficient, its value (0.161, 95%CI [0.079–0.243] for all diagnosis categories (Normal, PMS and PMDD) is still poorly agreed on between the DRSP and PSST [data not shown]. Additionally, when considering both coefficients comparing the normal and PMS/PMDD categories, the PABAK coefficient value (0.39) showed a moderate consistency between the DRSP and the PSST, although it still fits into a low intensity, according to Altman (1990).¹⁹19 Altman DG. Practical statistics for medical research. London: Chapman & Hall/CRC; 1990 The results of “normal versus PMS/PMDD diagnosis” and “PMS versus PMDD diagnosis” between the PSST and DRSP are displayed in Table 2.

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Table 2
Evaluation of PMS/PMDD diagnosis using the PSST

Discussion

Experts diverge about the most suitable PMS diagnostic tool. Many group members favored the DRSP; however, more simple methods are desirable for clinical use and for screening patients for research studies.¹¹11 O'Brien PM, Bäckström T, Brown C, et al. Towards a consensus on diagnostic criteria,measurement and trial design of the premenstrual disorders: the ISPMD Montreal consensus. Arch Women Ment Health 2011;14(01):13-21

The challenge for the diagnosis and classification of PMS is to distinguish women who need treatment from those without clinical relevance.²¹21 Bentz D, Steiner M, Meinlschmidt G. [SIPS-screening instrument for premenstrual symptoms. The German version of Premenstrual Symptoms Screening Tool to assess clinically relevant disturbances]. Nervenarzt 2012;83(01):33-39 The PSST is a fast and effective screening tool and an important starting point for further assessment.¹⁴14 Steiner M, Macdougall M, Brown E. The premenstrual symptoms screening tool (PSST) for clinicians. Arch Women Ment Health 2003;6(03):203-209

When comparing the data of the PSST with the results of the DRSP, our study shows that the PSST overestimated the diagnosis of PMDD and minimized the diagnosis of PMS. This may be explained by the fact that the PSST data was not collected over time.¹⁴14 Steiner M, Macdougall M, Brown E. The premenstrual symptoms screening tool (PSST) for clinicians. Arch Women Ment Health 2003;6(03):203-209 However, it is a good screening tool for PMS with a high sensitivity (79%).

This study points to an important conclusion: we had many losses; 135 women abandoned the recordkeeping, citing the amount of time taken to fulfill the record as a reason for the abandonment. The problem is that filling out the DRSP is a time-consuming process, which is frequently not followed through. An epidemiological study showed that 30% of women refused to participate in the study because they did not want to fill out a daily record. The recordkeeping in question may even cause resistance to future treatment offerings. Therefore, it is important to develop economic diagnostic tools for clinical practice.²¹21 Bentz D, Steiner M, Meinlschmidt G. [SIPS-screening instrument for premenstrual symptoms. The German version of Premenstrual Symptoms Screening Tool to assess clinically relevant disturbances]. Nervenarzt 2012;83(01):33-39

In a study with 1,477 women, only 56% completed the DRSP. This study included Brazilian women and showed an elevated incidence of moderate to severe PMS/PMDD: 47.7%.⁹9 Heinemann LA, Minh TD, Filonenko A, Uhl-Hochgräber K. Explorative evaluation of the impact of severe premenstrual disorders on work absenteeism and productivity. Womens Health Issues 2010;20(01):58-65 This demonstrates how difficult it is for women to keep a daily record as part of a research. In the clinical practice, the use of PMS/PMDD diaries is even less frequent.

This study has some limitations. Although 282 women completed the PSST, only 127 women returned with 2 cycles of DRSP filled out. This highlights the difficulty in the application of the DRSP in clinical practice and research, suggesting that the PSST should be used as the initial screening tool.

Conclusion

Considering that PMS/PMDD have a well-validated diagnostic tool, the DRSP, the PSST should be considered as a screening tool. The PSST underreported the PMS diagnosis and over-estimated the PMDD diagnosis. We recommend that positive cases of PMS/PMDD diagnosed by PSST are further evaluated by using the DRSP.

Acknowledgments

Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq, in the Portuguese acronym), Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES, in the Portuguese acronym) andFundode Incentivo à Pesquisa e Eventos/Hospital das Clínicas de Porto Alegre (FIPE/HCPA, in the Portuguese acronym) supported this research. We thank these institutions for their financial support and we would like to express our deepest gratitude to the participants for their time and patience throughout this study.

References

¹
Nillni YI, Rohan KJ, Zvolensky MJ. The role of menstrual cycle phase and anxiety sensitivity in catastrophicmisinterpretation of physical symptoms during a CO(2) challenge. Arch Women Ment Health 2012;15(06):413-422
²
Ryu A, KimTH. Premenstrual syndrome: Amini review.Maturitas 2015;82(04):436-440
³
Kessel B. Premenstrual syndrome. Advances in diagnosis and treatment. Obstet Gynecol Clin North Am 2000;27(03):625-639
⁴
Halbreich U, Borenstein J, Pearlstein T, Kahn LS. The prevalence, impairment, impact, andburdenofpremenstrualdysphoricdisorder (PMS/PMDD). Psychoneuroendocrinology 2003;28(Suppl 3):1-23
⁵
Rodrigues IC, Oliveira E. Prevalência e convivência demulheres com síndrome pré-menstrual. Arq Ciênc Saúde. 2006;13:146-152
⁶
Petta CA, Osis MJ, de Pádua KS, Bahamondes L, Makuch MY. Premenstrual syndrome as reported by Brazilian women. Int J Gynaecol Obstet 2010;108(01):40-43
⁷
Miller FC. Ten goals for the American College of Obstetricians and Gynecologists for the first decade of the next millennium. Obstet Gynecol 2000;95(01):1-5
⁸
Wittchen HU, Becker E, Lieb R, Krause P. Prevalence, incidence and stability of premenstrual dysphoric disorder in the community. Psychol Med 2002;32(01):119-132
⁹
Heinemann LA, Minh TD, Filonenko A, Uhl-Hochgräber K. Explorative evaluation of the impact of severe premenstrual disorders on work absenteeism and productivity. Womens Health Issues 2010;20(01):58-65
¹⁰
Nevatte T, O'Brien PM, Bäckström T, et al; Consensus Group of the International Society for Premenstrual Disorders. ISPMD consensus on the management of premenstrual disorders. ArchWomen Ment Health 2013;16(04):279-291
¹¹
O'Brien PM, Bäckström T, Brown C, et al. Towards a consensus on diagnostic criteria,measurement and trial design of the premenstrual disorders: the ISPMD Montreal consensus. Arch Women Ment Health 2011;14(01):13-21
¹²
Endicott J, Nee J, HarrisonW. Daily Record of Severity of Problems (DRSP): reliability and validity. ArchWomen Ment Health 2006;9 (01):41-49
¹³
Borenstein JE, Dean BB, Yonkers KA, Endicott J. Using the daily record of severity of problems as a screening instrument for premenstrual syndrome.ObstetGynecol 2007;109(05):1068-1075
¹⁴
Steiner M, Macdougall M, Brown E. The premenstrual symptoms screening tool (PSST) for clinicians. Arch Women Ment Health 2003;6(03):203-209
¹⁵
Spitzer RL, Kroenke K,Williams JB. Validation and utility of a selfreport version of PRIME-MD: the PHQ primary care study. Primary Care Evaluation of Mental Disorders. Patient Health Questionnaire. JAMA 1999;282(18):1737-1744
¹⁶
Fraguas R Jr, Henriques SG Jr, De Lucia MS, et al. The detection of depression in medical setting: a study with PRIME-MD. J Affect Disord 2006;91(01):11-17
¹⁷
American Psychiatric Association. Diagnostic and statistical manual of mental disorders: DSM-5. 5th ed.Washington, DC: American Psychiatric Publishing; 2013
¹⁸
Câmara RA, Köhler CA, Frey BN, Hyphantis TN, Carvalho AF. Validation of the Brazilian Portuguese version of the Premenstrual Symptoms Screening Tool (PSST) and association of PSST scores with health-related quality of life. Rev Bras Psiquiatr 2017;39(02):140-146
¹⁹
Altman DG. Practical statistics for medical research. London: Chapman & Hall/CRC; 1990
²⁰
Byrt T, Bishop J, Carlin JB. Bias, prevalence and kappa. J Clin Epidemiol 1993;46(05):423-429
²¹
Bentz D, Steiner M, Meinlschmidt G. [SIPS-screening instrument for premenstrual symptoms. The German version of Premenstrual Symptoms Screening Tool to assess clinically relevant disturbances]. Nervenarzt 2012;83(01):33-39

Publication Dates

Publication in this collection
Jan 2018

History

Received
22 Sept 2017
Accepted
05 Oct 2017

This is an open-access article distributed under the terms of the Creative Commons Attribution License

[1] ¹
Nillni YI, Rohan KJ, Zvolensky MJ. The role of menstrual cycle phase and anxiety sensitivity in catastrophicmisinterpretation of physical symptoms during a CO(2) challenge. Arch Women Ment Health 2012;15(06):413-422

[2] ²
Ryu A, KimTH. Premenstrual syndrome: Amini review.Maturitas 2015;82(04):436-440

[3] ³
Kessel B. Premenstrual syndrome. Advances in diagnosis and treatment. Obstet Gynecol Clin North Am 2000;27(03):625-639

[4] ⁴
Halbreich U, Borenstein J, Pearlstein T, Kahn LS. The prevalence, impairment, impact, andburdenofpremenstrualdysphoricdisorder (PMS/PMDD). Psychoneuroendocrinology 2003;28(Suppl 3):1-23

[5] ⁵
Rodrigues IC, Oliveira E. Prevalência e convivência demulheres com síndrome pré-menstrual. Arq Ciênc Saúde. 2006;13:146-152

[6] ⁶
Petta CA, Osis MJ, de Pádua KS, Bahamondes L, Makuch MY. Premenstrual syndrome as reported by Brazilian women. Int J Gynaecol Obstet 2010;108(01):40-43

[7] ⁷
Miller FC. Ten goals for the American College of Obstetricians and Gynecologists for the first decade of the next millennium. Obstet Gynecol 2000;95(01):1-5

[8] ⁸
Wittchen HU, Becker E, Lieb R, Krause P. Prevalence, incidence and stability of premenstrual dysphoric disorder in the community. Psychol Med 2002;32(01):119-132

[9] ⁹
Heinemann LA, Minh TD, Filonenko A, Uhl-Hochgräber K. Explorative evaluation of the impact of severe premenstrual disorders on work absenteeism and productivity. Womens Health Issues 2010;20(01):58-65

[10] ¹⁰
Nevatte T, O'Brien PM, Bäckström T, et al; Consensus Group of the International Society for Premenstrual Disorders. ISPMD consensus on the management of premenstrual disorders. ArchWomen Ment Health 2013;16(04):279-291

[11] ¹¹
O'Brien PM, Bäckström T, Brown C, et al. Towards a consensus on diagnostic criteria,measurement and trial design of the premenstrual disorders: the ISPMD Montreal consensus. Arch Women Ment Health 2011;14(01):13-21

[12] ¹²
Endicott J, Nee J, HarrisonW. Daily Record of Severity of Problems (DRSP): reliability and validity. ArchWomen Ment Health 2006;9 (01):41-49

[13] ¹³
Borenstein JE, Dean BB, Yonkers KA, Endicott J. Using the daily record of severity of problems as a screening instrument for premenstrual syndrome.ObstetGynecol 2007;109(05):1068-1075

[14] ¹⁴
Steiner M, Macdougall M, Brown E. The premenstrual symptoms screening tool (PSST) for clinicians. Arch Women Ment Health 2003;6(03):203-209

[15] ¹⁵
Spitzer RL, Kroenke K,Williams JB. Validation and utility of a selfreport version of PRIME-MD: the PHQ primary care study. Primary Care Evaluation of Mental Disorders. Patient Health Questionnaire. JAMA 1999;282(18):1737-1744

[16] ¹⁶
Fraguas R Jr, Henriques SG Jr, De Lucia MS, et al. The detection of depression in medical setting: a study with PRIME-MD. J Affect Disord 2006;91(01):11-17

[17] ¹⁷
American Psychiatric Association. Diagnostic and statistical manual of mental disorders: DSM-5. 5th ed.Washington, DC: American Psychiatric Publishing; 2013

[18] ¹⁸
Câmara RA, Köhler CA, Frey BN, Hyphantis TN, Carvalho AF. Validation of the Brazilian Portuguese version of the Premenstrual Symptoms Screening Tool (PSST) and association of PSST scores with health-related quality of life. Rev Bras Psiquiatr 2017;39(02):140-146

[19] ¹⁹
Altman DG. Practical statistics for medical research. London: Chapman & Hall/CRC; 1990

[20] ²⁰
Byrt T, Bishop J, Carlin JB. Bias, prevalence and kappa. J Clin Epidemiol 1993;46(05):423-429

[21] ²¹
Bentz D, Steiner M, Meinlschmidt G. [SIPS-screening instrument for premenstrual symptoms. The German version of Premenstrual Symptoms Screening Tool to assess clinically relevant disturbances]. Nervenarzt 2012;83(01):33-39

Variables	(n= 127)
Age (years) - Mean ± SD [Min-Max]	33.7 ± 6.6 [20.0–45.0]
Skin color - n (n%)
White	112 (88.2)
Not white	15 (11.8)
Educational level - n (n%)
Elementary	3 (2.4)
High school	37 (29.1)
Academic	85 (66.9)
Using non-continuous regimens of combined hormonal contraceptive - n (n%)
Yes	72 (56.7)
No	55 (43.3)
Smoker - n (n%)
Yes	4 (3.1)
No	123 (96.9)
BMI - n (n%)
Normal	59 (46.5)
Overweight	44 (34.6)
Obese	24 (18.9)

Variables	Normal versus PMS/PMDD diagnosis	PMS versus PMDD diagnosis
Sensitivity [95%CI]	79.00% [70.02%–85.83%]	60.00% [23.07%–88.24%]
Specificity [95%CI]	33.33% [18.64%–52.18%]	59.46% [48.08%–69.91%]
Positive Predictive value [95%CI]	81.40% [76.68%–85.42%]	9.1% [4.34%–18.06%]
Negative Predictive value [95%CI]	30.00% [18.32%–45.02%]	95.7% [88.46%–98.44%]
Kappa [95%CI]	0.119 [−0.068–0.305]	0.054 [−0.076–0.184]
p	0.181	0.393
PABAK	0.39	0.19

Brasil

Brasil

Premenstrual Syndrome Diagnosis: A Comparative Study between the Daily Record of Severity of Problems (DRSP) and the Premenstrual Symptoms Screening Tool (PSST)

Diagnóstico de síndrome pré-menstrual: um estudo comparativo entre o relato diário da gravidade dos problemas (DRSP) e o instrumento de rastreamento de sintomas pré-menstruais (PSST)

Abstract

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Introduction

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Acknowledgments

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History