Analysis of pathological features related to clinical prognosis in C3 glomerulopathy

doi:10.16150/j.1671-2870.2024.06.005

Abstract

Abstract:

Objective To analyze pathological features related to clinical prognosis in C₃ glomerulopathy. Methods A total of seven cases diagnosed as C₃ nephropathy by renal biopsy in the Department of Nephrology, Ruijin Hospital, Shanghai Jiao Tong University School of Medicine from 2012 to 2022 were collected. The clinical, pathological and follow-up data were retrospectively analyzed, and the prognostic pathological features were observed. Results Among the 7 patients (male/female, 3/4), the median onset age was 51 years, the median age at diagnosis was 54 years, and the median follow-up time was 84 months (ranging from 48 to 144 months). Two patients were lost to follow-up, 2 patients showed poor prognosis, and 3 patients had good prognosis. Clinically, 2 cases presented with nephrotic syndrome, 3 cases had renal insufficiency, and 6 cases had hematuria. All 7 patients exhibited hypocomplementemia and hypertension, with no obvious extrarenal manifestations. Among the 5 patients with long-term follow-up, by the 2-year follow-up, 1 patient had complete remission of proteinuria and creatinine levels, 3 patients had stable proteinuria and renal function, and 1 patient had increased proteinuria and declining renal function. By the 6-year follow-up, 3 patients had good prognosis, 1 patient who had poor prognosis at the 2-year follow-up showed further increase in proteinuria and significant decline in renal function, and 1 patient progressed to massive proteinuria. At the 6-year follow-up, a retrospective analysis of renal pathology revealed that 3 cases with good prognosis primarily exhibited diffuse endothelial cell proliferation with neutrophil infiltration, with minimal glomerular sclerosis and faint double-track appearance of the capillary loops. In these cases, there was also limited deposition of electron-dense material in the mesangial area.. Two cases with poor prognosis showed an increased proportion of glomerular sclerosis, extensive double-track appearance of capillary loops, and significant deposition of electron-dense material in the mesangial area, while endothelial cell proliferation with neutrophil and eosinophil infiltration was less pronounced. Conclusions Acute pathological changes (such as glomerular capillary endothelial cell proliferation and neutrophil infiltration) are the main manifestations of C₃ nephropathy, which is associated with a good prognosis and can be treated aggressively with steroids and immunosuppressants. The pathological manifestations of C₃ are mainly chronic lesions (including glomerular sclerosis, double-track formation of capillary loops, and extensive deposition of electron-dense material in the mesangial area). C₃ patients have poor prognosis, and conservative treatment is recommended to avoid excessive treatment.

Key words: C₃ glomerulopathy, Clinical manifestation, Renal pathology, Prognosis

CLC Number:

R692
R446.8

ZHANG Junhua, LI Yilin, XIE Jingyuan, ZHANG Chunli, XU Jing. Analysis of pathological features related to clinical prognosis in C₃ glomerulopathy[J]. Journal of Diagnostics Concepts & Practice, 2024, 23(06): 587-593.

Figures/Tables 3

Table 1

Table 2

Figure 1

References 20

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Index	case1	case2	case3	case4	case5	case6	case7
Baseline data
Gender	Female	Female	Female	Female	Male	Male	Male
Age of onset（years）	51	42	58	18	54	58	26
Age at diagnosis（years）	51	54	64	23	57	58	29
Follow up（months）	3	108	48	72	144	84	0
Family history	No	No	No	No	No	No	No
SP（mmHg）	137	118	128	120	124	180	138
DP（mmHg）	81	90	89	74	86	96	85
NS	No	No	Yes	No	No	No	Yes
24 h TUP（mg）	2274	1632	4092	1508	877	1538	6301
Microscopic hematuria（/HP）	11-15	6-11	4-5	Full field	6-10	4-5	0
Scr（μmol/L）	175	55	102	47	94	113	78
eGFR（mL/min）	28.6	114.5	49.2	134.1	79．8	61.4	116
sAlb（g/L）	25	26	26	30	30	33	29
C₃（g/L）	0.28	0.06	0.6	0.6	0.56	0.62	0.43
C₄（g/L）	0.1	0.1	0.18	0.12	0.12	0.2	0.18
Hb（g/L）	119	113	92	108	115	122	150
Therapy	MMF+P	ARB+P	ARB+P+CYC	ARB	ARB+P+MMF	ARB	ARB+P+CYC
Remission time（months）	3	3	2	3	32	No	NA
Relapse（months）	NA	18	No	46	67	No	NA
Follow up for 2 years data
Therapy	NA	ARB+P+CNI	ARB	ARB	ARB+P+MMF	ARB+P+MMF	NA
24 h TUP（mg）	NA	1542	155	954	352	2273	NA
Scr（μmol/L）	NA	62	78	54	100	157	NA
eGFR（ml/min）	NA	991	68.1	142.1	72.6	43.25	NA
sAlb（g/L）	NA	29	42	33	35	27	NA
C₃（g/L）	NA	0.06	NA	0.08	0.64	NA	NA
C₄（g/L）	NA	0.1	NA	0.1	0.1	NA	NA
Follow up for 6 years data
Therapy	NA	ARB+P+CNI	NA	ARB	ARB+P+RTX	ARB+P+MMF	NA
24 h TUP（mg）	NA	1236	NA	354	6013	3627	NA
Scr（μmol/L）	NA	69	NA	51	131	202	NA
eGFR（mL/min）	NA	96	NA	126.9	53.5	29.2	NA
sAlb（g/L）	NA	29	NA	39	17	26	NA
C₃（g/L）	NA	0.07	NA	0.46	0.59	NA	NA
C₄（g/L）	NA	0.1	NA	0.2	0.2	NA	NA

Index	case1	case2^*	case3^*	case4^*	case5	case6	case7
LM
Glomerulus（n）	36	6	33	29	19	22	39
Glomerulosclerosis（n,%）	2(5.6)	0(0)	3(9)	0(0)	3(15.8)	5(26.3)	12(30.8)
Proportion of glomerulosclerosis increased	0	0	0	0	0	1	1
Segmental sclerosis（n）	2	0	0	2	0	0	5
Endocapillary proliferation	1	1	1	1	0	0	0
Neutrophils in capillaries	1	1	1	1	0	0	0
Capillary loop double track	0	0	0	0	1	1	1
Mesangial matrix increased	3	3	3	3	2	3	3
Mesangial cells increased	1	3	3	3	2	3	2
Interstitial fibrosis	1	1	1	1	1	2	2
Tubules atrophic	1	1	1	1	1	2	2
Interstitial inflammatory cell	1	1	3	1	1	2	2
IF
Deposition of C₃	2	3	3	3	2	2	2
other immune complexes	0	1	0	1	0	1	0
EM
Electron dense deposits
Mesangial zone	1	1	1	0	3	2	2
Epithelial side	0	1	1	0	0	0	2
Subepithelial	0	0	1	1	1	2	2
GBM	0	0	1	0	0	0	2
Foot process fusion	1	1	1	0	1	0	1

Analysis of pathological features related to clinical prognosis in C₃ glomerulopathy

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