Table 1

Overview of clinical, radiological, scintigraphic, and molecular data on patients from the 24 families

	Family 1	Family 2	Family 3	Family 4	Family 5
	(Belgium)	(Iraq)	(UK)	(Italy)	(Belgium)
Mutation (DNA)	673T→C	653G→A	652C→T	28_36dup	241T→C
Mutation (protein)	C225R	R218H	R218C	L10-L12dup	Y81H
Number of patients	3	5	3	2	3

Clinical symptoms	3/3	4/5	2/3	2/2	1/3
Pain in extremities	2/3	4/5	2/3	0/2	1/3
Easy fatigability	0/3	3/5	2/3	0/2	1/3
Muscle weakness	0/3	2/5	2/3	0/2	1/3
Waddling gait	1/3	3/5	1/3	0/2	1/3
Hearing loss	0/3	2/5	0/3	2/2	0/3
Reduced subcutaneous fat	1/3	2/5	0/3	2/2	1/3
Other	Hyperthermia (1/3)	Hepatosplenomegaly (1/3)	ESR and CRP↑ (2/3)	–	Small stature (1/3)
		Cranial nerve compression (1/3)
		Small stature (2/3)
		Headache (1/3)

Radiological abnormalities	3/3	5/5	3/3	2/2	1/3
Cortical thickening diaphyses	3/3	5/5	3/3	2/2	1/3
Sclerosis of skull	1/3	2/5	ND	2/2	0/3
Other	–	–	Spine osteoporotic (2/3)	Spine, pelvis (1/2)	–
			Coxa valga (2/3)

Increased BMD	ND	ND	+ (hip) (2/3)	2/2	ND
			− (spine) (2/3)

Scintigraphic abnormalities	ND	4/4	ND	1/1	1/1

Treatment	GC (1/3)	GC (1/5)	GC (2/3)	Calcitonin (1/2)	GC (1/3)
	NSAIDs (1/3)		NSAIDs (2/3)	BP (2/2)	NSAIDs (1/3)
			Analgesics (2/3)		Analgesics (1/3)
			BP (2/3)
			Tibial osteotomy (1/3)
			Femoral osteotomy (1/3)

	Family 6	Family 7	Family 8	Family 9	Family 10
	(Belgium)	(Italy)	(Germany)	(UK)	(Tonga-Oceania)
Mutation (DNA)	241T→C	653G→A	653G→A	653G→A	653G→A
Mutation (protein)	Y81H	R218H	R218H	R218H	R218H
Number of patients	6	2	3	2	2

Clinical symptoms	3/6	2/2	1/3	1/2	1/2
Pain in extremities	2/6	1/2	1/3	1/2	0/2
Easy fatigability	1/6	1/2	1/3	0/2	0/2
Muscle weakness	1/6	1/2	1/3	0/2	0/2
Waddling gait	2/6	2/2	1/3	0/2	0/2
Hearing loss	0/6	0/2	0/3	0/2	1/2
Reduced subcutaneous fat	0/6	1/2	0/3	0/2	0/2
Other	–	–	–	–	Proptosis (1/2)

Radiological abnormalities	4/6	2/2	1/1	2/2	2/2
Cortical thickening diaphyses	4/6	2/2	1/1	2/2	2/2
Sclerosis of skull	1/2	0/2	ND	ND	1/1
Other	Pelvis (1/2)	–	–	ND	–

Increased BMD	ND	ND	ND	ND	1/1

Scintigraphic abnormalities	1/6	ND	1/1	ND	1/1

Treatment	GC (1/6)	–	Penicillin	Treated with vitamin D for presumed rickets (1/2)	Orbital decompression (1/1)
	BP (1/6)		Gold salts
			NSAIDs

	Family 11	Family 12	Family 13	Family 14	Family 15*
	(Morocco)	(Belgium)	(Spain)	(Germany)	(Israel)
Mutation (DNA)	463C→T	673T→C	652C→T	664C→G	652C→T
Mutation (protein)	R156C	C225R	R218C	H222D	R218C
Number of patients	2	3	4	1	16

Clinical symptoms	2/2	2/3	4/4	1/1	10/16
Pain in extremities	2/2	2/3	2/4	1/1	8/8
Easy fatigability	1/2	1/3	0/4	1/1	ND
Muscle weakness	0/2	1/3	4/4	1/1	4/8
Waddling gait	1/2	1/3	1/4	1/1	6/8
Hearing loss	0/2	0/3	0/4	0/1	0/8
Reduced subcutaneous fat	Obese (2/2)	Obese (1/3)	0/4	1/1	ND
Other	ESR and CRP↑ (1/2)	–	Vision ↓ (1/4)	Delayed puberty	Inability to run quickly (3/8)
	ESR and CRP↑ (1/2)		Mild splenomegaly (2/4)	Small stature	Inability to run quickly (3/8)
			Recurrent facial paralysis (1/4)
			Hypertension (1/4)

Radiological abnormalities	2/2	3/3	4/4	1/1	11/11
Cortical thickening diaphyses	2/2	3/3	4/4	1/1	11/11
Sclerosis of skull	0/2	0/3	4/4	0/1	ND
Other	Enlarged mandible (1/2)	Kyphoscoliosis (1/3)	Pelvis (3/4)	Genu valgum	ND
	Enlarged mandible (1/2)	Coxa valga (1/3)	Spine (1/4)	Pes valgus
			Vertebrae (1/4)	Coxa valga

Increased BMD	ND	ND	ND	ND	ND


Scintigraphic abnormalities	2/2	1/2	4/4	ND	ND

Treatment	Analgesics (2/2)	NSAIDs (2/3)	GC (1/4)	–	?
	GC (2/2)

	Family 16†	Family 17‡	Family 18‡	Family 19‡	Family 20‡
	(Japan)	(Portugal)	(France)	(Belgium)	(France)
Mutation (DNA)	673T→C	653G→A	652C→T	673T→C	673T→C
Mutation (protein)	C225R	R218H	R218C	C225R	C225R
Number of patients	12	12	2	3	3

Clinical symptoms	10/12	10/12	2/2	2/3	2/3
Pain in extremities	10/12	10/12	2/2	2/3	2/3
Easy fatigability	ND	8/12	1/2	2/3	2/3
Muscle weakness	7/12	7/12	1/2	2/3	2/3
Waddling gait	5/12	7/12	1/1	1/3	2/3
Hearing loss	3/12	ND	ND	ND	ND
Reduced subcutaneous fat	ND	ND	ND	ND	ND
Other	Marfanoid habitus (3/12)	Headache (2/12) Poor appetite (2/12)	Poor appetite (1/2)		Headache (3/3) Poor appetite (1/3)
	Facial nerve palsy (1/12)	Delayed puberty (?)
	Delayed puberty (1/1)
	Delayed puberty (1/1)

Radiological abnormalities	12/12	10/10	ND	3/3	3/3
Cortical thickening diaphyses	12/12	10/10	ND	3/3	3/3
Sclerosis of skull	3/12	9/11	ND	ND	1/2
Other	ND	ND	ND	ND	ND



Increased BMD	ND	8/10	2/2	3/3	3/3

Scintigraphic abnormalities	1/1	ND	ND	ND	ND

Treatment	?	GC (1/12)	?	?	?

	Family 21‡	Family 22‡	Family 23‡	Family 24§
	(Australia)	(France)	(France)	(USA)	Summary
This family has been described by Janssens et al*.¹²
†This family has been described by Makita et al.⁹
‡These families have been described by Campos-Xavier et al.¹⁰
§This family has been described by Wallace et al.¹¹
?, Data not available; –, data absent; ↑, increased; ↓, decreased.
BMD, bone mineral density; BP, bisphophonates; CRP, C reactive protein; ESR, erythrocyte sedimentation rate; GC, glucocorticoids; ND, not determined; NSAIDs, non-steroidal anti-inflammatory drugs.
Mutation (DNA)	673T→C	652C→T	652C→T	653G→A
Mutation (protein)	C225R	R218C	R218C	R218H
Number of patients	2	1	2	6	100

Clinical symptoms	2/2	1/1	2/2	4/6	74/100 (74%)
Pain in extremities	2/2	1/1	2/2	3/6	63/92 (68%)
Easy fatigability	2/2	1/1	1/2	3/6	32/72 (44%)
Muscle weakness	1/2	1/1	1/2	4/6	36/92 (39%)
Waddling gait	1/2	1/1	1/2	4/6	44/92 (48%)
Hearing loss	ND	ND	ND	2/6	10/67 (15%)
Reduced subcutaneous fat	ND	ND	ND	2/6	10/47 (21%)–3/47 (6%) obese
Other	Headache (2/2) Poor appetite (2/2)	Poor appetite	Headache (1/2) Poor appetite (1/2)	Vertigo, tinnitus, balance problems (2/6)
				Delayed puberty (1/6)
				Poor appetite (1/6)
				Facial paralysis (1/6)

Radiological abnormalities	2/2	1/1	2/2	3/4	82/87 (94%)
Cortical thickening diaphyses	2/2	1/1	2/2	3/4	82/87 (94%)
Sclerosis of skull	2/2	1/1	2/2	3/4	32/59 (54%)
Other	ND	ND	ND	Enlarged mandible (1/6)	Pelvis 5/8 (63%)
				Genu valgum (3/6)
				Pes planus (3/6)

Increased BMD	2/2	1/1	2/2	ND	26/29 (90%)


Scintigraphic abnormalities	ND	ND	ND	ND	17/23 (74%)

Treatment	?	?	?	GC (2/6)
				Hip surface replacement (1/6)
				Tibial, fibular, and femoral osteotomy (1/6)