Clinical Findings

The clinical history from each patient is outlined in the following paragraphs and key clinical and laboratorial findings are summarized in Tables 1 and 2. Patient 1 was a 40-year-old woman that had started, at the age of 35, having frequent falls and progressive difficulty climbing stairs. Patient 2 was a 36-year-old woman that reported that she did not speak until she was 4 years old and, at the age of 24, started having upper left arm weakness. Patient 3 was a 15-year-old girl that presented with frequent falls and difficulty walking and climbing stairs. Patient 4 was a 28-year-old woman that had started, in childhood, losing the incapacity to run and progressive difficulty climbing stairs. Patient 5 was a 26-year-old woman admitted with a history of elbow joint contractures since childhood, at age of 16 she started having difficulties raising from chairs, and at age of 18 started having myalgia, difficulties climbing stairs, and raising her arms. Patient 6 was a 68-year-old woman admitted with generalized myalgia and cramps since the age of 58; at age 63, she started having lumbar pain, frequent falls, and difficulties climbing stairs; she had dyslipidemia and had used statins for several years. Patient 7 was a 44-year-old woman with the inability to climb stairs without support since age 38; at age 44, she started having difficulties raising her arms. Patient 8 was a 33-year-old woman that had started, at the age of 12, having a progressively abnormal gait, frequent falls, and difficulty standing up; at age 33, she started having difficulty climbing stairs and raising her arms. Patient 9 was a 48-year-old woman with abnormal, unstable gait and difficulty running and climbing stairs; at age 46, she began having frequent falls and difficulties raising her arms. Patient 10 was a 42-year-old woman that had acquired independent gait at the age of 3, and, at the age of 28, started progressive gait abnormality, cramps, and difficulty climbing stairs.

Table 1

Clinical presentation in a series of symptomatic dystrophinopathy carriers

Age=age at admission; calf (+)=increased calf volume; NA=not available; NR=not reported; start: age at first symptoms.

Table 2

Ancillary investigation in a series of symptomatic dystrophinopathy carriers

Serum creatine kinase times increase referent to each age-dependent reference values.

Imaging age=age at image studies and time elapsed between first symptoms and imaging examination; mosaic=dystrophin immunohistochemistry with positive and negative or decreased intensity fibers; NR=not reported.

Five patients (1, 2, 3, 5, and 6) were initially submitted for muscle biopsy with immunohistochemistry before subsequent molecular investigation. Five patients (4, 7-10) were not submitted for muscle biopsy and their diagnosis was confirmed by clinical, imaging, and molecular correlations.

Patients’ ages at admission ranged from 15 to 68 years, with a mean of 38.1 years. The age range of first symptoms varied from the ages 2 to 58, with a mean of 27.8 years (Table 1). Half of the patients did not present any affected male relatives (Table 1). Gowers maneuver was present in seven of eight patients, and patient 5 presented with early elbow contractures at initial clinical presentation (Table 1). Serum creatine kinase levels varied from 648 to 4509 IU/l, which corresponded to a ratio of 3.9 to 27.3 times the respective reference values, with a mean increase of 9.7 times the reference values (Table 2). Creatine kinase levels are higher in younger patients than in older patients, when necrotic process of muscle fibers is active.

Imaging Studies

Patients 1, 3, 5, 7, and 8 underwent computed tomography scanning at the time of the investigation. Patient 6 underwent magnetic resonance imaging (MRI) on 1.5-Tesla equipment, including coronal and axial T1-weighted sequences, coronal and axial short T1 inversion recovery sequences, and axial fat-saturated T2-weighted sequences. Muscle imaging studies demonstrated predominant asymmetric muscle fat replacement (Figures 1 and 2, Table 2). Severe muscle fat replacement was observed as follows.

• ∙ Patient 1: bilateral medial, posterior, and anterior thigh; bilateral medial gastrocnemius; and left soleus

• ∙ Patient 3: bilateral glutei, bilateral adductor magnus, bilateral vastus intermedius, and left vastus lateralis

• ∙ Patient 5: right vastus lateralis, left quadriceps femoris, bilateral adductor magnus, bilateral biceps femoralis, left semimembranosus, bilateral soleus, bilateral peroneus, left gastrocnemius lateralis, and left gastrocnemius medialis

• ∙ Patient 6: right gluteus maximus, bilateral adductor magnus, bilateral semimembranosus, and right medial gastrocnemius

• ∙ Patient 7: right vastus lateralis, bilateral biceps femoris, right semitendinosus, right semimembranosus, bilateral adductor magnus, and left medial gastrocnemius

• ∙ Patient 8: bilateral vastus lateralis, bilateral vastus intermedius, left rectus femoralis, left biceps femoralis, left semitendinosus, left semimembranosus, bilateral soleus, left medial gastrocnemius, and right lateral gastrocnemius.

Figure 1

Muscle image studies: predominant asymmetric muscle fat replacement of pelvis, thigh, and legs. (A) Patient 1 CT, (B) patient 3 CT, (C) patient 5 CT, (D) patient 6 magnetic resonance imaging, (E) patient 7 CT, and (F) patient 8 CT.

Figure 2

Schematic diagram of the pelvis, thighs, and legs. am=adductor magnus; bf=biceps femoris; g=gracilis; gl=gastrocnemius lateralis; gm=gastrocnemius medialis; Gmax=gluteus maximus; Gmed=gluteus medius; Gmin=gluteus minimus; p=peroneus; rf=rectus femoris; s=sartorius; sm=semimembranosus; so=soleus; st=semitendinosus; ta=tibialis anterior; vi=vastus intermedius; vl=vastus lateralis, vm=vastus medialis.

The most commonly involved muscle groups were glutei and thigh adductors, followed by posterior and anterior thigh and posterior leg muscles. Patients 1 and 8 presented the most severe muscle fat replacement, which corresponded to them having with the longest duration of symptoms: 14 and 21 years of disease progression, respectively (Figure 1, Table 2). All patients, except patient 1, presented sartorius and gracilis muscles preservation compared with other muscle groups.

Muscle Biopsy

Muscle biopsy was performed in patients 1, 2, 3, 5, and 6. A myopathic pattern was demonstrated in all patients, with a variation in fiber caliber. Immunohistochemical studies with serial sections with dystrophin-spectrin were performed, because spectrin is a marker of muscle fiber membrane integrity. Dystrophin immunohistochemistry demonstrated clear mosaic pattern in two patients (1 and 2) and only subtle reduction of dystrophin intensity in three patients (3, 5, and 6) (Figure 3). The intensity of dystrophin expression was compared with both preservation of spectrin expression in the same group of fibers in serial sections and intensity of dystrophin expression compared with normal fibers and control muscle (Figure 3).

Figure 3

Muscle biopsy of patient 6. (A) Variation in fiber caliber with atrophy (arrow) and hypertrophy (arrow head) (hematoxylin and eosin [HE], 100×). (B) Rimmed vacuole (arrow) (HE 400×). (C, D) Serial sections (arrows) of muscle fibers with decreased dystrophin immunohistochemical expression and preservation of spectrin expression. (C) dystrophin carboxy terminal DYS2 200×; (D) spectrin 200×). (E) Filamentous inclusions (arrow). (F) Myofibrillar loss and accumulation of dense matrix mitochondria (arrow). (E, F) Transmission electron microscopy 15,000×, 6000×.

Molecular Studies

All patients underwent molecular investigation and all presented dystrophin gene deletions (Table 2). The deletions were found in DMD gene exons 13, 13-17, 20-29, 20-41, 38-43, 45, 45-46, 46-55, 47-48, and 48-50 (Table 2). Heterozygous c.1554T>A, p.D518E missense mutation in exon 13, to the best of our knowledge, has not been previously described. This mutation was associated with immunohistochemical dystrophin mosaic pattern and considered functionally pathogenic (patient 3)(Table 2).