多发性硬化症的临床和认知进展中种族和性别交叉。
The intersection of race and sex on the clinical and cognitive progression of multiple sclerosis.
机构信息
Department of Neurology | School of Medicine, Louisiana State University Health Sciences Center, New Orleans, LA, USA.
Department of Cellular Biology and Anatomy, Medical College of Georgia at Augusta University, Augusta, GA, USA.
出版信息
J Neurol Sci. 2024 Nov 15;466:123260. doi: 10.1016/j.jns.2024.123260. Epub 2024 Sep 26.
OBJECTIVE
Black populations show increased incidences of diagnosis, worse disease severity, and earlier likelihood of mortality due to MS. Clinical outcomes are also linked to biological sex and as with Black individuals, MS characteristics between sexes have also shifted overtime. This study examined whether clinical disease progression differed by race and sex for patients with MS.
DESIGN
"Black" (N = 47) and "White" (N = 58) participants with MS (82 % female) were recruited from a longitudinal examination of the impact of race and sex on the cognition and disease duration of patients in the gulf south region of the United States.
RESULTS
Black participants had shorter disease durations [F (1,103) = 4.70, p = .03], (MDiff = [-3.96]) and were younger [F (1, 103) = 14.25, p < .001], (MDiff = [-9.04]). Despite this, Black individuals had worse SDMT t-scores [F (1, 103) = 5.22, p = .024], (MDiff = [-4.62])]. Women exhibited higher MSSS scores [F (1, 96) = 5.59, p = .02], (MDiff = [-2.15]). Specifically, Black women were younger than White women [F (1, 84) = 14.47, p < .001], (MDiff = [-9.15])] and had shorter disease durations [F (1, 84) = 6.04, p = .016], (MDiff = [-4.57])] yet scored lower on the SDMT T-scores [F (1, 84) = 6.11, p = .015], (MDiff = [-5.51])].
CONCLUSION
Findings suggest an interaction between race and sex may influence clinical progression in MS. Despite being younger and having shorter disease durations Black participants with MS, specifically Black women exhibited worse clinical outcomes.
SUMMARY
For women and men, MS incidence among Black Americans has become similar to White Americans. However, Black individuals experience greater disease severity and earlier mortality. Clinical impairment often accompanies MS. We examined the influence of race and sex on clinical status using the Symbol Digit Modalities Test t-scores (SDMT T-scores) and Multiple Sclerosis Severity Scores (MSSS) in Black (N = 47) and White (N = 58) patients with MS. Women exhibited higher MSSS scores than men [F (1, 96) = 5.59, p = .02], (MDiff = [-2.15]). Black participants had shorter disease durations [F (1, 103) = 4.70, p = .03], (MDiff = [-3.96]) and were younger [F (1, 103) = 14.25, p < .001], (MDiff = [-9.04]). Despite this, Black individuals had worse SDMT T-scores [F (1, 103) = 5.22, p = .024], (MDiff = [-4.62])]. Specifically, Black women were younger than White women [F (1, 84) = 14.47, p < .001], (MDiff = [-9.15])] and had shorter disease durations [F (1, 84) = 6.04, p = .016], (MDiff = [-4.57])] yet scored lower on the SDMT T-scores [F (1, 84) = 6.11, p = .015], (MDiff = [-5.51])]. These findings suggest that an interaction between race and sex may influence clinical progression in MS.
目的
黑人群体在多发性硬化症的诊断、疾病严重程度和死亡率方面的发生率更高。临床结果也与生物学性别有关,与黑人一样,多发性硬化症的性别特征也随时间发生了变化。本研究检查了多发性硬化症患者的种族和性别是否会影响疾病的临床进展。
设计
“黑人”(N=47)和“白人”(N=58)参与者(82%为女性)来自美国海湾南部地区对种族和性别对患者认知和疾病持续时间影响的纵向研究。
结果
黑人参与者的疾病持续时间更短[F(1,103)=4.70,p=0.03],(MDiff=[-3.96])且更年轻[F(1,103)=14.25,p<.001],(MDiff=[-9.04])。尽管如此,黑人个体的 SDMT t 评分更差[F(1,103)=5.22,p=0.024],(MDiff=[-4.62])]。女性的 MSSS 评分更高[F(1,96)=5.59,p=0.02],(MDiff=[-2.15])]。具体来说,黑人女性比白人女性更年轻[F(1,84)=14.47,p<.001],(MDiff=[-9.15])]且疾病持续时间更短[F(1,84)=6.04,p=0.016],(MDiff=[-4.57])],但 SDMT t 评分更低[F(1,84)=6.11,p=0.015],(MDiff=[-5.51])]。
结论
研究结果表明,种族和性别之间的相互作用可能会影响多发性硬化症的临床进展。尽管黑人多发性硬化症患者更年轻,疾病持续时间更短,但黑人参与者的临床结局更差。多发性硬化症常伴有临床损伤。我们使用符号数字模态测试 t 评分(SDMT t 评分)和多发性硬化症严重程度评分(MSSS),检查了种族和性别对黑人(N=47)和白人(N=58)多发性硬化症患者临床状况的影响。女性的 MSSS 评分高于男性[F(1,96)=5.59,p=0.02],(MDiff=[-2.15])]。黑人参与者的疾病持续时间更短[F(1,103)=4.70,p=0.03],(MDiff=[-3.96])且更年轻[F(1,103)=14.25,p<.001],(MDiff=[-9.04])]。尽管如此,黑人个体的 SDMT t 评分更差[F(1,103)=5.22,p=0.024],(MDiff=[-4.62])]。具体来说,黑人女性比白人女性更年轻[F(1,84)=14.47,p<.001],(MDiff=[-9.15])]且疾病持续时间更短[F(1,84)=6.04,p=0.016],(MDiff=[-4.57])],但 SDMT t 评分更低[F(1,84)=6.11,p=0.015],(MDiff=[-5.51])]。这些发现表明,种族和性别之间的相互作用可能会影响多发性硬化症的临床进展。
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